Zoonotic Babesia: A scoping review of the global evidence
Authors:
Kaitlin M. Young aff001; Tricia Corrin aff001; Barbara Wilhelm aff002; Carl Uhland aff003; Judy Greig aff001; Mariola Mascarenhas aff001; Lisa A. Waddell aff001
Authors place of work:
Public Health Risk Sciences Division, National Microbiology Laboratory, Public Health Agency of Canada, Guelph, Ontario, Canada
aff001; Big Sky Health Analytics, Vermilion, Alberta, Canada
aff002; Independent Consultant, St-Hyacinthe, Quebec, Canada
aff003
Published in the journal:
PLoS ONE 14(12)
Category:
Research Article
doi:
https://doi.org/10.1371/journal.pone.0226781
Summary
Background
Babesiosis is a parasitic vector-borne disease of increasing public health importance. Since the first human case was reported in 1957, zoonotic species have been reported on nearly every continent. Zoonotic Babesia is vectored by Ixodes ticks and is commonly transmitted in North America by Ixodes scapularis, the tick species responsible for transmitting the pathogens that also cause Lyme disease, Powassan virus, and anaplasmosis in humans. Predicted climate change is expected to impact the spread of vectors, which is likely to affect the distribution of vector-borne diseases including human babesiosis.
Methods
A scoping review has been executed to characterize the global evidence on zoonotic babesiosis. Articles were compiled through a comprehensive search of relevant bibliographic databases and targeted government websites. Two reviewers screened titles and abstracts for relevance and characterized full-text articles using a relevance screening and data characterization tool developed a priori.
Results
This review included 1394 articles relevant to human babesiosis and/or zoonotic Babesia species. The main zoonotic species were B. microti, B. divergens, B. duncani and B. venatorum. Articles described a variety of study designs used to study babesiosis in humans and/or zoonotic Babesia species in vectors, animal hosts, and in vitro cell cultures. Topics of study included: pathogenesis (680 articles), epidemiology (480), parasite characterization (243), diagnostic test accuracy (98), mitigation (94), treatment (65), transmission (54), surveillance (29), economic analysis (7), and societal knowledge (1). No articles reported predictive models investigating the impact of climate change on Babesia species.
Conclusion
Knowledge gaps in the current evidence include research on the economic burden associated with babesiosis, societal knowledge studies, surveillance of Babesia species in vectors and animal hosts, and predictive models on the impact of climate change. The scoping review results describe the current knowledge and knowledge gaps on zoonotic Babesia which can be used to inform future policy and decision making.
Keywords:
Database searching – Zoonoses – Epidemiology – Infectious disease surveillance – Ticks – Babesia – Vector-borne diseases – Babesiosis
Introduction
Babesiosis is a vector-borne disease caused by infection with erythrocytic protozoal parasites of the genus Babesia. There are over 100 species of Babesia, many of which are well-established threats to domestic animals and livestock [1, 2]. Only a few species are known to be capable of causing infection in humans [3]. Since the first case of human babesiosis was reported in 1957 in a Croatian splenectomised farmer [4], zoonotic Babesia species have been reported on nearly every continent. In North America, B. microti is the most reported cause of infection, with the majority of cases originating from the Northeast and upper Midwest United States [5]. In Europe, B. divergens remains the most frequent cause of human babesiosis [6]. Other zoonotic species that have been reported in the literature include B. duncani and B. venatorum, in addition to other related and unnamed Babesia.
Zoonotic Babesia species are vectored by ticks of the genus Ixodes [2] and require a mammalian reservoir host, such as the white-footed mouse, to complete their life cycle. The presence of different Babesia species around the world is dependent on the geographic distribution of competent vectors. The most common vectors of zoonotic Babesia species are Ixodes scapularis, I. ricinus, and I. persulcatus ticks in North America, Europe, and Asia, respectively [7]. Transmission to humans can occur from the bite of an infected tick [8], through the passage of contaminated blood via transfusions [9–12], or transplacentally from infected mother to fetus [13]. Typically, infection is asymptomatic and self-limiting in healthy persons. Common mild symptoms include flu-like manifestations such as fever, chills, headache, fatigue, loss of appetite, nausea, and shortness of breath. Elderly, splenectomised, and other immunocompromised individuals are at a higher risk of severe symptomology and may experience hemolytic anemia, splenomegaly, hepatomegaly, renal failure, and even death. Infection is usually diagnosed through microscopic examination of blood smears with Babesia species characterized largely by their size and appearance. It is recommended that patients with mild to moderate babesiosis are treated with combination therapy of atovaquone and azithromycin and severe cases with clindamycin and quinine [14, 15]. As no vaccine currently exists, tick avoidance through personal protective measures such as repellants, protective clothing, and tick checks are recommended, especially in areas of tick endemicity [2].
Evidence suggests that Ixodes tick ranges are changing in part due to climate change. As an example, in Canada the I. scapularis range has been expanding and cases of babesiosis, Lyme disease, Powassan virus, and anaplasmosis are increasingly being reported in affected areas [16].
In response to the potential for expansion in Canada, a scoping review (ScR) was conducted to capture the global evidence on babesiosis and Babesia species that infect humans. The aim was to identify and characterize the existing research on this topic, create a repository of the published literature, and identify any knowledge gaps that may facilitate decision-making on this public health issue in North America. Several literature reviews on zoonotic Babesia have been published; however, to the best of our knowledge, this is the only ScR that utilizes a systematic and reproducible methodology to present an updated overview of the zoonotic Babesia literature.
Methods
Review protocol and expertise
The ScR protocol was created a priori to ensure reproducible, transparent, and consistent results. The protocol, which includes a list of definitions, search algorithms, abstract screening form, and data characterization and utility form, can be found in the supplementary information (S1 Protocol). The repository of relevant articles and resulting dataset is also available (S1 Dataset).
Creation of the protocol and execution of the review was completed by a team of individuals with multi-disciplinary expertise in epidemiology, public health, knowledge synthesis, risk assessment, vector-borne diseases, and information science.
Review question and scope
The objective of this ScR was to identify relevant evidence that addresses the broad research question: What are the characteristics of the global evidence on human babesiosis and zoonotic Babesia species?
Search strategy
A comprehensive search strategy using the algorithm (babesiosis and (human or humans or man or woman or people)) or (Babesia), was executed in the following bibliographic databases on February 20, 2017 and updated May 10, 2018: PubMed, Scopus, Cochrane Library, and Global Health/EMBASE. There was no constraint on publication date for this search.
To ensure an exhaustive repository of relevant articles, the capacity of the electronic search was verified by hand searching the reference lists of ten literature reviews focused or partially focused on babesiosis in humans [2, 17–25]. From this exercise, six peer-reviewed primary literature articles were identified and added to the ScR for evaluation and characterization.
An extensive complementary search for grey literature, defined in this review as materials and research produced by organizations outside of the traditional commercial or academic publishing and distribution channels (e.g. government reports of surveillance data), was conducted in Google using the algorithms employed in the electronic search. A ‘snowball’ search technique was utilized in examining the first 100 hits. Using the same search terms and algorithms as described above, targeted government country and provincial/state websites were searched. For Canada and the United States, states/provinces from which the review captured reports of human babesiosis cases were then the subject of online searches for notification/monitoring systems. European, Asian, and South American countries captured by the initial electronic database search were investigated through Google using the algorithm (Country) AND (Babesia), as well as searching within the regional Centers for Disease Control and health (e.g. Pan-American Health Organization) websites. Finally, the specialized electronic bibliographic databases OpenGrey [26] and DataCite [27] were searched for relevant grey literature. Ultimately, 22 additional references were added to the project from the grey literature search.
Relevance screening and inclusion criteria
A relevance screening form was developed a priori to encompass the inclusion and exclusion criteria of the ScR. Abstracts, titles, and keywords were screened for relevance using the following question: Does this citation describe primary research on babesiosis in humans or a Babesia species that is pathogenic to humans (in vectors, hosts, humans, or a parasite in-vitro study) or a predictive model examining the impacts of climate change on Babesia/babesiosis? Due to limited translation resources, articles published in languages other than English or French were excluded.
Study characterization and extraction
Full-text articles of potentially relevant citations were reviewed using the data characterization and utility form. This form was developed a priori and designed to confirm article relevance, study design, population, outcomes, data utility, and capture whether the article addressed the impacts of climate change on the parasite.
Scoping review management, data charting, and analysis
Citations found by the search strategy were imported into the reference management software, EndNote (EndNote X7, Clarivate Analytics), where duplicates were removed. These citations were then imported into the online electronic systematic review management platform DistillerSR (DistillerSR, Evidence Partners, Ottawa, Canada), where all stages of the ScR, including relevance screening and data characterization, were completed independently by two reviewers. Any conflicts that arose were mediated by a third reviewer.
Data collected from the data characterization and utility form were exported to Excel (Excel 2010, Microsoft Corporation, Redmond, WA), for formatting and descriptive analysis (frequencies and percentages). This process facilitated categorization and charting of relevant findings.
Results
Descriptive statistics
After an extensive literature search and de-duplication process, 7537 abstracts and titles were screened for relevance from which 2610 full-text articles were reviewed. A total of 1394 relevant research articles (English = 1368 and French = 26) on zoonotic Babesia were characterized in this ScR (Fig 1 and S1 Dataset). Exclusions due to language (n = 136 articles) included: Chinese (n = 23), Czech (3), Danish (n = 2), Dutch (n = 5), German (n = 45), Hebrew (n = 1), Hungarian (n = 1), Italian (n = 3), Japanese (n = 5), Polish (n = 6), Portuguese (n = 2), Russian (n = 12), Serbo-Croatian (n = 1), Spanish (n = 20), Swedish (n = 1), and Turkish (n = 6) (S1 Exclusions). The major foci of these excluded articles were pathogenesis (n = 35), epidemiology (n = 45), in vitro Babesia studies (n = 13), transmission (n = 6), mitigation (n = 5), treatment (n = 4), and diagnostic test accuracy (n = 4). We were unable to identify a study focus for 29 excluded articles due to limited information in English or French. Relevant articles were published between 1957 and 2018, with 65% (901/1394) published since the year 2000. The majority of these articles were peer-reviewed research (1304/1394) and most frequently covered topics on pathogenesis (signs, symptoms, and diagnosis) (680/1394), and epidemiology (480/1394). Articles utilized observational (845/1394) or experimental (532/1394) study designs to investigate zoonotic Babesia (Table 1). Individual articles discussed throughout this ScR could have reported the results of one or more studies. Conference proceedings (n = 65), grey literature (n = 19), theses (n = 4), and predictive models (n = 2) containing primary data made up a small percentage of the articles included.
Other foci of study included in vitro, in silico, and molecular morphology of zoonotic Babesia parasites (i.e. parasite characterization) (243/1394), articles evaluating mitigation strategies or interventions (94/1394), evaluation of diagnostic tests (98/1394), investigation of treatments (65/1394), studies on transmission or parasite competence (54/1394), description of Babesia surveillance activities (29/1394), economic burden or cost-benefit analysis (7/1394), and social impacts and knowledge (1/1394) (Fig 2). There were no articles captured on predictive models investigating the impact of climate change on Babesia species. All definitions of study characteristics, categories, and outcomes can be found in the included ScR protocol (S1 Protocol).
Bubble size is proportional to number of articles. Articles could have had more than one study focus.
Humans were sampled in 534 articles (534/1394), of which 368 were case series or case reports (Table 1). Cattle were the most frequently sampled animal hosts (59/215) followed by 33 articles on bank voles, a common host of Ixodes species in Europe [28] and 22 articles on white-footed mice, which are cited as a common reservoir species for Babesia in North America [2]. There were 375/1394 articles that reported studies investigating Babesia using animal model species (Table 2), while 179/1394 reported the examination of parasites using cell culture methods. Ticks were the only vectors investigated (266/1394).
Evidence of the capacity for human infection was identified for seven Babesia species (Table 1). These included B. microti, B. divergens, B. duncani, B. venatorum, B. microti-like, B. divergens-like, and B. crassa-like. There are also several variants that have been associated with human infection but remain unnamed. These include B. sp. KO1, B. sp. TW1, B. sp. MO1, B. sp. CA1, B. sp. WA2 (aka B. duncani-type), and B. sp. XXB/HangZhou. From here, reference to Babesia species refers to only those known to infect humans (i.e. zoonotic).
Babesia characterization
Babesia characterization, meaning studies of the parasite(s) with no affiliation to a host, was the focus of 243/1394 articles. Cell cultures were used to investigate parasite pathogenesis, including immune reactions and production of various antigens/antibodies (77/243), as well as to examine the transmission characteristics of the parasite that facilitate movement from one host to another (e.g. receptors and proteins) (9/243). The genetic makeup of the pathogen to determine relatedness of isolates and/or identify key areas of conservation or mutation was reported in 182/243 articles. Many of these articles reported phylogenetic trees (114/182) and/or whole genome sequencing (7/182) in their study analyses.
Molecular epidemiology, which examines the link between epidemiological information and genetics of the pathogen, was the focus of two articles (2/243) [29, 30].
Transmission routes and scenarios
In articles that reported on human sampling frames (534/1394), tick bites were the most common reported source of exposure to Babesia (155/534), followed by blood transfusion (78/534). Four studies reported human exposure through direct contact with infected animals or tick infested animals [31–34]. Transplacental transmission of B. microti in humans from mother to fetus has been reported in ten studies. Two of these were surveillance reports [5, 35] and eight were case reports describing newborns with congenital infections [36–43]. None of the infants were reported to have long-term sequelae from the congenital B. microti infection. The source of exposure was not described in 349/534 articles that sampled humans.
Blood transfusion transmission scenarios were studied in two experiments. In a challenge study, Rhesus macaque monkeys were used to investigate parasitemia kinetics and immune responses following transfusion of blood infected with B. microti [44]. Another challenge study analyzed the viability of B. microti infected blood stored at room temperature or 4°C [45].
Conditions for transmission of zoonotic Babesia species to, from, and between humans, animals, or vectors was the focus of 54/1394 articles. Host-to-host transmission scenarios were reported in 8/54 of the transmission articles. These included observational studies that documented transplacental transmission in naturally-infected populations of white-footed mice and meadow voles in endemic areas of the United States [46], as well as common voles, tundra voles, and field voles in Poland [47]. Similarly, transplacental transmission has also been demonstrated experimentally in a population of BALB/c lab mice [48]. Other host-to-host studies described experimental attempts at the induction of infection through inoculation of infected blood from cattle to reindeer [49], cattle to sika deer [50], macaque to macaque [44], and between desert woodrats, dusty-footed woodrats, California voles, California mice, and deer mice [51]. One study, published in 1994, demonstrated oral transmission of Babesia through oral gavage and cannibalism in laboratory mice [52].
Host to vector (21/54) and vector to host (22/54) transmission scenarios involved the experimental feeding of ticks on infected animals, or infected ticks on Babesia-free animals (S1 Table). These studies examined whether sufficient parasitemia was reached in animal species to transmit Babesia to ticks and whether various tick species were competent vectors of zoonotic Babesia species. Many of these studies also monitored infection kinetics throughout the course of infection.
Only 15/54 of the transmission articles specifically reported on the competency of vectors to transmit Babesia. The most frequent outcome was transmission potential defined as the presence of the parasite within the salivary gland of the tick (12/15), demonstrated by B. microti in I. scapularis [8, 53–58]; B. venatorum [59], B. divergens [60], and B. microti in I. ricinus [61, 62]; and B. microti in I. ovatus and I. persulcatus [63]. Competency studies also investigated the course of B. microti metamorphosis in the gut of I. scapularis ticks [58, 64, 65] and B. divergens metamorphosis in the gut of I. ricinus ticks [60], as well as the ability of B. microti to cross the peritrophic membrane in I. scapularis ticks [66].
Vector to vector transmission (7/54) included investigations of transstadial and/or transovarial transmission of B. microti in I. ricinus (2/7), I. trianguliceps (1/7), D. andersonii (1/7) and R. heamaphysaloides (1/7) and B. divergens in I. ricinus (2/7).
Diagnostic testing and accuracy
Many studies captured in this review utilized a form of testing for the purpose of either identifying Babesia in patients, animals, and ticks, screening host populations for antibodies indicative of prior infection, or for the evaluation of their accuracy in diagnosing human cases and/or detecting Babesia species in non-human hosts.
Blood samples were taken in 94.6% (505/534) of articles reporting human sampling frames to determine Babesia infection or sero-positivity in humans. Evidence of Babesia infection was also demonstrated in the erythrocytes of the spleen [67–70], kidney [71], lymph node, lung, and liver [69], as well as in the bone marrow [4, 72–83], cerebral spinal fluid [84–87], placenta [37], and amniotic fluid [42] of patients. Microscopic blood smear evidence of Babesia was the most common method of diagnosis in humans (407/534), followed by immunoassay (302/534) and molecular (235/534) techniques. In 64/534 articles, infection status was investigated using whole animal bioassays.
In articles that reported animal sampling frames (natural hosts and animal model species), diagnosis involved microscopic blood smear examinations (422/567), immunoassays (191/567), and molecular techniques (156/567). Molecular methods were most heavily relied on for the identification of Babesia in ticks (230/266), while 35/266 articles reported microscopic bodily fluid exams and 4/266 immunoassays.
There were 98/1394 articles that had a diagnostic test accuracy focus. These articles reported on the accuracy of one or more diagnostic/detection tests, of which 19/98 reported on microscopic examination and staining of Babesia parasites in blood (n = 17), tissue (n = 1), and bodily fluid (n = 1). Serological test accuracy, including indirect fluorescent antibody technique and enzyme-linked immunosorbent assay, was reported in 48/98 articles. Molecular test accuracy, most frequently concerning polymerase chain reaction, was reported in 46/98 articles. Notably, only 53.1% (52/98) of these articles provided extractable outcome data on the sensitivity, specificity, and/or raw data on the test accuracy.
Pathogenesis in humans and animal hosts
Pathogenesis was the focus of 680/1394 articles. Humans were studied in 390/680 of these articles, of which 368/390 were case series or case reports. These studies investigated the course of Babesia infection, diagnosis, clinical characteristics, and complications. Five articles also reported on the immune response elicited by infection (5/390). Signs and symptoms of disease manifestation were reported in most of the human articles (365/390), while pathology outcomes, defined as any blood, urine, or tissue results using chemistry, clinical microbiology, hematology, or molecular pathology to characterize the progression of disease, were reported in less than half (181/390). Post-mortem findings (14/390) and chronic sequelae resulting from babesiosis infection (4/390) were rarely mentioned in the literature. The intrinsic incubation period, also known as the time between infection and the onset of symptoms, was reported in 6/390 articles.
Challenge or controlled trials were used to investigate pathogenesis in experimental animal models (266/680). In addition to describing the course of Babesia infection (160/266), these experiments were used to investigate the infection mechanism (19/266) and immune response (131/266) in the animal. These trials allowed investigators to study infection characteristics including signs and symptoms (68/266), the latent period (139/266), intrinsic incubation period (2/266), and infectious period (7/266) of the experimental animal model species.
Animal case reports provided results of pathology (4/20) and post-mortem examinations (3/20). Specific signs and symptoms of animals naturally infected with Babesia were reported in over half of the case reports (11/20). No long-term sequelae were reported in any of the animal studies.
Coinfections
Many articles reported coinfection (209/1394) of zoonotic Babesia with other pathogens. Coinfections were noted in 124/534 articles that reported on humans. These included case reports (77/124), cohort studies (4/124), case-control studies (2/124), cross-sectional studies (18/124), prevalence surveys (22/124), surveillance programs (6/124), and a longitudinal study (1/124) that identified the presence of Babesia and other pathogens. Lyme disease, caused by Borrelia burgdorferi, was the most common coinfection (99/124) followed by ehrlichiosis (17/124), anaplasmosis (15/124), bartonellosis (3/124), and rickettsioses (2/124). One article (1/124) reported coinfection with two or more Babesia species simultaneously [88].
Of the articles that reported on animal host populations in which zoonotic Babesia were detected, 30/173 reported at least one coinfection as an outcome. These included the bacteria; Borrelia (8/30), Anaplasma (8/30), Bartonella (5/30), Ehrlichia (4/30), Grahamella (1/30), Candidatus (2/30), Leptospira (1/30), parasites; two or more species of Babesia (6/30), Trypanosoma (2/30), Hepatozoon (1/30), Theileria (6/30), and the virus; Dobrava-Belgrade Virus (1/30).
Of the articles that reported on tick populations in which zoonotic Babesia species were detected, 57/211 reported at least one coinfection as an outcome. These included coinfections with multiple species of Borrelia (43/57), Anaplasma (21/57), Ehrlichia (4/57), Rickettsia (16/57), Theileria (1/57), Bartonella (1/57), Tick-borne Encephalitis Virus (2/57), Toxoplasma gondii (3/57), Coxiella burnetii (1/57), and Candidatus Neoehrlichia mikurensis (3/57).
Epidemiology
Epidemiology was the focus of 480/1394 articles. Babesia infection or exposure in humans was reported in 137/480 epidemiology articles (Table 3). Most of these articles (76/137) reported general population sampling frames (e.g. blood donors or random sample of people in an area), fewer reported an “at risk” population (45/137) such as forestry workers, farmers, or individuals with a history of tick bites, or cases of clinically diagnosed babesiosis (20/137) in an area (usually a state/province) in a defined time period. Cross-sectional (45/137) and prevalence surveys (58/137) were the most popular study designs used for gathering human epidemiological data. Case prevalence, identification of the number of individuals with Babesia infection in a sampling frame, was a reported outcome among populations in 46/137 articles. Other outcomes included seroprevalence (89/137) and incidence (31/137). Statistically significant risk factors for exposure to Babesia were communicated in 28/137 articles reporting on epidemiological studies of human populations. In addition to the epidemiological studies, 372/1394 articles described human sporadic cases, with hospitalizations and/or case-fatalities reported in 332/372 and 52/372 articles, respectively (Table 3).
Epidemiology articles that reported zoonotic Babesia in animal hosts reported case prevalence (140/173), seroprevalence (46/173), and incidence (2/173) (Table 4 and S2 Table). Prevalence surveys were the most common epidemiological study captured (92/173), followed by cross-sectional (74/173), longitudinal (7/173), cohort (5/173), and surveillance or monitoring program (3/173). Nineteen articles (19/1394) reported sporadic cases of babesiosis within animal host populations (Table 4), of which 4/19 reported case fatalities.
Among the epidemiology articles, 211/480 reported evidence of zoonotic Babesia infection in at least one tick species. Ticks were primarily collected by the use of tick dragging (149/211), which involves dragging a white cloth over vegetation to collect questing ticks. Other articles described obtaining ticks through removal from human or animal hosts (89/211) for testing. Across epidemiology articles, all life stages were collected, however nymph (148/211) and adult (161/211) life stages were more frequently sampled than larvae (67/211).
The majority of epidemiology articles reported infection in the Ixodes genus of ticks (Table 5). Babesia was also detected in the following tick populations: Dermacentor reticulatus [89–96], D. marginatus [97–99], D. sylvarum [100], Haemaphysalis longicornis [101–103], H. punctata [98, 99, 104], H. concinna [100, 105, 106], H. leporispalustris [107], H. japonica [108], H. sulcata [109], Hyalomma marginatum [110, 111], Amblyomma variegatum [112], Argas (Carios) vespertilionis [113], Rhipicephalus simus [114], R. turanicus [115], R. bursa [116], R. microplus [101], and R. sanguineus [117]. Five articles (5/211) estimated the minimum infection rate within tick species [63, 107, 118–120].
Surveillance
Surveillance to determine the extent of Babesia infection in a population was the focus of 29/1394 articles. The majority of the articles were concerned with human infections (23/29). Many relied on passive surveillance wherein physicians report disease cases to state level public health authorities (18/23). Other data collection strategies included active surveillance (3/23) or monitoring programs (2/23). Reports of human babesiosis surveillance were identified from the United States (22/23) and Manitoba, Canada (1/23) [121].
Animal hosts were the subject of active surveillance in 3/29 articles. These reported zoonotic Babesia infection in voles [122] and white-footed mice [123] in the United States, as well as seropositive red foxes in Italy [124].
Tick surveillance for Babesia was reported in 7/29 articles. European surveillance studies investigated I. ricinus tick species in Italy [124], and I. ariadnae, I. vespertilionis, and I. simplex in Hungary and Romania [125]. North American studies included 3/7 in the United States [126–128] and 2/7 in Canada [121, 129].
Treatment
Babesia treatments were the focus of 65/1394 articles. Only 2/65 of these articles reported on human treatments. A prospective randomized trial investigated the efficacy of a regimen of atovaquone and azithromycin compared to a regimen of clindamycin and quinine [14]. Another studied the efficacy of atovaquone and cholestyramine combination therapy [130]. Treatments were also investigated in 46/65 animal experiments and 29/65 in vitro anti-parasitic experiments. The most common drugs investigated were Imidocarb dipropionate (17/65), Quinine (13/65), Atovaquone (13/65), Diminazene aceturate (12/65), Clindamycin (12/65), Chloroquine (9/65), Pentamidine (8/65), and Azithromycin (6/65).
Mitigation
Mitigation efforts to prevent and/or control zoonotic Babesia were the focus of 94/1394 articles. Interventions for human blood supply safety (20/94), such as screening protocols and tests, were investigated most frequently in the United States (16/20). The impact of pyrethroid-impregnated ear tags for prophylaxis of B. divergens in cattle was studied in two controlled trials (2/94). Vaccine candidates were explored in 52/94 articles, including 50/52 challenge trials and 3/52 controlled trials using animals. Animal models and in vitro studies also examined the impact of adoptive transfer of immunity and various inhibitory chemicals, prophylactic antimicrobials, and microorganisms on Babesia or the likelihood of developing Babesia infection (20/94).
Preventative control strategies including human behavioural measures, public education to decrease the probability of tick contact for humans and companion animals, landscape modification, and biological control of the vector, were not assessed in any of the zoonotic Babesia literature.
Societal knowledge
Only one article (1/1394) focused on societal knowledge of babesiosis or zoonotic Babesia species. Canadian physicians were surveyed to gather information about their knowledge of transfusion-transmitted infection risks and current reporting practices for tick-borne diseases, including babesiosis [131].
Economic analysis
Seven articles (7/1394) focused on different aspects of the economic impact of babesiosis. One study estimated the median hospitalization costs of babesiosis in Spain [132] and another the costs of tick-borne disease laboratory diagnostic testing in the United States [133]. Cost effectiveness of sampling and laboratory analyses strategies were evaluated in one study using total cost reduction calculations in Italy [134]. The cost-benefit of B. microti blood donation screening techniques was estimated using quality-adjusted life years in three studies within the United States [135–137]. Another study in the United States evaluated the cost implications of pathogen inactivation for donated platelets [138].
Discussion
Babesia has been prioritized as a disease of public health importance in Canada due to the potential for expansion with climate change. To provide a robust and comprehensive synthesis, we summarized the characteristics of the global evidence on zoonotic Babesia. Our intention is that the available literature and knowledge gaps discussed herein will support evidence-informed decision-making on this issue. The findings provide a detailed narrative of the literature available on a global scale, while the discussion has an emphasis on the characteristics, mitigation, and natural transmission of Babesia in North America. Since the first case of human babesiosis was reported in 1957, research on zoonotic Babesia has steadily increased, particularly under the foci of pathogenesis and epidemiology. However, other important avenues of study such as societal knowledge and economic analyses have seldom been undertaken.
Babesia microti, B. divergens, B. duncani, and B. venatorum are among the named species that cause the majority of human cases, and thus are commonly discussed in the literature on babesiosis. Based on their morphology, most of these Babesia are sub-categorized as “small Babesia” which are closely related to Theileria species and include B. microti, B. duncani, B. venatorum, and B. microti-like, as well as the non-zoonotic species B. gibsoni and B. rodhaini. There are also large Babesia which consist of B. sp. KO1 [139] and the non-zoonotic species B. bovis, B. cabelli, B. vogeli, and B. canis [2]. B. divergens is a special case in that microscopically it appears to be a small Babesia, but shares a closer genetic lineage to large Babesia species [2].
Despite these morphological differences, classification and diagnosis of Babesia can present a particular challenge for physicians and laboratory personnel. Microscopically, many species are indistinguishable from each other and are difficult to differentiate from other plasmodial diseases (i.e. malaria). Commercially available serologic tests may have variable sensitivity and specificity and are not reliable for distinguishing between Babesia species. Reliably distinguishing between some Babesia species that are morphologically and serologically indistinguishable such as B. duncani and B. microti requires the use of molecular tests (e.g. polymerase chain reaction) to confidently identify the species [140]. From a public health perspective it is unclear if treatment efficacy differs by species of Babesia as currently, treatment depends on the severity of disease rather than species of Babesia causing the infection. As vectors and hosts are often shared by a multitude of infectious agents, coinfection with other vector-borne diseases, such as Lyme disease, is not uncommon in areas of endemicity [141, 142]. Coinfections should be considered during diagnosis to ensure appropriate treatment is administered in a timely manner, especially since there is the potential for coinfections to lead to more severe illness [142, 143].
It is also important that physicians are aware of the various routes of human exposure to Babesia and collect a thorough patient history regarding recent travel, exposure to ticks, and possible parasite exposure through transfusion or transplants. For example, only 7.2% of Canadian family physicians surveyed in 2002 were aware that babesiosis can be transmitted through blood transfusion [131]. With the incidence of tick-borne disease expected to increase in Canada in the coming years in part due to climate change, an updated survey of both physician and the general population would be helpful in elucidating the current state of knowledge and in guiding future public health promotion and preparedness activities.
There are several common treatments for babesiosis in humans. The majority of mild to moderate babesiosis cases are treatable with combination therapy of atovaquone and azithromycin [14, 130]. Recommendations for treatment of severe babesiosis include the use of clindamycin and quinine combination therapy [15, 144], which is not recommended for treatment of mild to moderate illness due to the risk of adverse reactions [14]. A number of risk factors have been associated with severe Babesia infections which may require long or repeated antibiotic therapy [2, 145, 146] and B. divergens has been associated with severe cases that require adjunct therapies such as red blood cell exchange [147, 148]. Analytic studies investigating the recalcitrance and virulence of Babesia species would provide useful evidence for steering treatment decisions. Prescribers and physicians must remain mindful of appropriate treatment regimens that minimize the risk of adverse health risk to patients as well as the potential for antimicrobial drug resistance to arise [149]. Such outcomes could ultimately result in prolonged duration of infection and hospitalization, resulting in increased healthcare expenditure. The economic impact of babesiosis has not been estimated in North America, however an article from Spain calculated the median cost per hospitalized case to be approximately $4710.86 USD [132].
This ScR identified a small number of reports of babesiosis in Canada, which included three human cases designated as locally-acquired [150, 151], three travel acquired cases [152–155], and a transfusion-transmitted case [156]. Babesiosis is not a reportable disease in Canada and only became a reportable disease in 18 of the United States in 2011, 1124 cases were reported that year [5]. However, this disease may currently be underreported as evidence of exposure to Babesia based on seroprevalence data from endemic regions of the United States ranges from 6%-16% [157, 158]. In North America, B. microti is frequently reported in the general immunocompetent population [144], whereas in Europe the majority of clinical cases have been attributed to B. divergens and have mostly been limited to asplenic individuals [159]. The surveillance data captured out of the United States indicates that there has been an increasing incidence of babesiosis over time [5]; however, like many vector-borne diseases it is unclear whether the rise in reported cases can be attributed to a general increased awareness of the disease, better diagnostic methods, or an actual increased risk of human exposure to Babesia. Cohort studies utilizing large sample sizes would be beneficial in gauging risk factors and incidence of infection.
Mitigation efforts in the literature have mainly focused on vaccinations and protecting the blood supply. Babesia is considered one of the leading infectious disease threats to blood supplies in the United States, with 165 cases of transfusion-transmitted B. microti infections reported between 1979 to 2016 [126, 160]. In Canada, there has been only one case of transfusion-transmitted babesiosis, reported in 1999 [156]. No laboratory screening program is in effect for donations in Canada or the United States [161]. Current donor screening and deferral is based upon a self-reported questionnaire question about babesiosis history, which is not a sensitive screening strategy as many infected individuals are asymptomatic [129]. Economic models indicated that donor screening assays may be cost-effective in endemic areas with a high infection prevalence [135, 137]. However, in many areas of the United States screening programs are not considered cost-effective due to the low transmissibility, short acute course, and low mortality associated with Babesia infection [136]. In Canada, a seroprevalence survey conducted in 2013 found no positive antibody responses to B. microti in Canadian blood donors; thus, there was insufficient evidence to warrant a screening program [129]. A second study is underway with 50,000 Canadian blood donors from across the country to provide a more comprehensive and up-to-date risk assessment of Babesia in the blood supply [162]. No human behavioural protective measures or environmental interventions such as landscape modification or chemical control measures (e.g. acaricides) were studied for their efficacy in reducing zoonotic babesiosis. However, multiple studies have investigated these interventions for their efficacy in reducing vectors (I. scapularis) with or without a focus on other pathogens (e.g. lyme disease) [163]. Because these interventions broadly aim to reduce human exposure to these ticks, it is reasonable to conclude they would be effective in reducing the transmission of all pathogens harboured by the targeted tick species, including Babesia.
The North American enzootic cycle of B. microti and the natural transmission between its main vector I. scapularis and reservoir host, the white footed mouse, has been well documented in the literature [2, 164], as has the natural transmission of B. divergens between I. ricinus and bovine hosts in Europe [148, 165]. Other reservoirs of Babesia have not been well characterized but may include other rodents, lagomorphs, and cervids [165]. While there has been no evidence of horizontal transmission between animal hosts reported, transplacental transmission has been demonstrated for white-footed mice [46], meadow voles [46] and common voles [47] and may partially explain the high prevalence of B. microti in endemic sites [46]. This ScR identified evidence confirming the competence of I. scapularis, I. ricinus, I. ovatus, and I. persulcatus as vectors of B. microti and/or B. divergens [8, 53–61, 63–66, 166], which is in agreement with the belief that the majority of vectors of zoonotic Babesia species are Ixodes ticks [2]. However, for other zoonotic Babesia species such as B. duncani, the reservoir host(s) and tick vector(s) are an area of active research in order to close knowledge gaps [167]. Further epidemiological and experimental research to examine the transmission of these emerging parasites is essential in understanding the enzootic and zoonotic transmission cycles.
The results of this ScR characterize the current evidence and knowledge gaps pertaining to babesiosis and Babesia infection. Rigorous efforts were made to capture all relevant literature on the topic; however, there is a possibility that some research evaded identification due to publication bias or absence of indexing. Due to limited translation resources, articles published in any language other than English and French were not characterised in this ScR. This may have resulted in an under-representation of research from some countries which may bias the results of zoonotic Babesia research from these areas. The aim of a ScR is to provide an overview of all of the research conducted on a broad topic. A risk of bias of the evidence included is not conducted in a ScR, instead the goal is to identify all relevant research. Thus, the readers should be aware that a wide range of studies is included in the ScR. The field of zoonotic Babesia research, including implications for clinical and policy-making practice, would benefit from systematic review(s) of the evidence that address the feasibility and effectiveness of certain treatments, mitigation practices, and resource-using activities such as surveillance and intervention. This ScR has provided an all-encompassing overview of the literature that can help aid in shaping such focused research questions appropriate for systematic review.
There were many evidence gaps identified in this ScR which included few epidemiological studies in certain geographic areas where zoonotic Babesia circulate or are likely to emerge. Thus, further epidemiological and surveillance work may be warranted to monitor the potential emergence of Babesia into previously unaffected areas. Keeping apprised of the emergence and burden of Babesia, diagnosis, treatment, and effective mitigation strategies is important to inform future policy and decision making on this issue and guide public health mitigation programs.
Supporting information
S1 Protocol [docx]
Protocol and search strategies employed for our scoping review on the characteristics of the global evidence of babesiosis and zoonotic .
S1 Dataset [xlsx]
List of references and full data characterization dataset analyzed in our scoping review on the characteristics of the global evidence of babesiosis and zoonotic .
S1 Exclusions [xlsx]
References excluded from our scoping review due to language.
S1 Table [docx]
Table of host to vector and vector to host transmission scenarios captured in our scoping review.
S2 Table [docx]
Table of animal epidemiology outcomes and sporadic case reports captured in our scoping review.
Zdroje
1. Levine ND. Progress in taxonomy of the Apicomplexan protozoa. J Protozool. 1988;35(4):518–20. doi: 10.1111/j.1550-7408.1988.tb04141.x 3143826
2. Homer MJ, Aguilar-Delfin I, Telford SR Iii, Krause PJ, Persing DH. Babesiosis. Clin Microbiol Rev. 2000;13(3):451–69. doi: 10.1128/cmr.13.3.451-469.2000 10885987
3. Vannier E, Gewurz BE, Krause PJ. Human babesiosis. Infect Dis Clin North Am. 2008;22(3):469–88, viii–ix. doi: 10.1016/j.idc.2008.03.010 18755385
4. Skrabalo Z, Deanovic Z. Piroplasmosis in man; report of a case. Doc Med Geogr Trop. 1957;9(1):11–6. 13427667
5. Herwaldt BL, Montgomery S, Woodhall D, Bosserman EA. Babesiosis surveillance—18 states, 2011. MMWR Morb Mortal Wkly Rep. 2012;61(27):505–9. 22785341
6. Gray J, Zintl A, Hildebrandt A, Hunfeld KP, Weiss L. Zoonotic babesiosis: overview of the disease and novel aspects of pathogen identity. Ticks Tick Borne Dis. 2010;1(1):3–10. doi: 10.1016/j.ttbdis.2009.11.003 21771506
7. Vannier E, Krause PJ. Human Babesiosis. N Engl J Med. 2012;366(25):2397–407. doi: 10.1056/NEJMra1202018 22716978
8. Piesman J, Spielman A. Human babesiosis on Nantucket Island: prevalence of Babesia microti in ticks. Am J Trop Med Hyg. 1980;29(5):742–6. doi: 10.4269/ajtmh.1980.29.742 7435782
9. Lobo CA, Cursino-Santos JR, Alhassan A, Rodrigues M. Babesia: an emerging infectious threat in transfusion medicine. PLoS Pathog. 2013;9(7):e1003387. doi: 10.1371/journal.ppat.1003387 23853577
10. Leiby DA. Transfusion-associated babesiosis: shouldn’t we be ticked off? Ann Intern Med. 2011;155(8):556–7. doi: 10.7326/0003-4819-155-8-201110180-00363 21893616
11. Gubernot DM, Lucey CT, Lee KC, Conley GB, Holness LG, Wise RP. Babesia infection through blood transfusions: reports received by the US Food and Drug Administration, 1997–2007. Clin Infect Dis. 2009;48(1):25–30. doi: 10.1086/595010 19035776
12. Gubernot DM, Nakhasi HL, Mied PA, Asher DM, Epstein JS, Kumar S. Transfusion-transmitted babesiosis in the United States: summary of a workshop. Transfusion. 2009;49(12):2759–71. doi: 10.1111/j.1537-2995.2009.02429.x 19821952
13. Fox LM, Wingerter S, Ahmed A, Arnold A, Chou J, Rhein L, et al. Neonatal babesiosis: case report and review of the literature. Pediatr Infect Dis J. 2006;25(2):169–73. doi: 10.1097/01.inf.0000195438.09628.b0 16462298
14. Krause PJ, Lepore T, Sikand VK, Gadbaw J Jr., Burke G, Telford SR 3rd, et al. Atovaquone and azithromycin for the treatment of babesiosis. N Engl J Med. 2000;343(20):1454–8. doi: 10.1056/NEJM200011163432004 11078770
15. Wormser GP, Dattwyler RJ, Shapiro ED, Halperin JJ, Steere AC, Klempner MS, et al. The clinical assessment, treatment, and prevention of lyme disease, human granulocytic anaplasmosis, and babesiosis: clinical practice guidelines by the Infectious Diseases Society of America. Clin Infect Dis. 2006;43(9):1089–134. doi: 10.1086/508667 17029130
16. McPherson M, Garcia-Garcia A, Cuesta-Valero FJ, Beltrami H, Hansen-Ketchum P, MacDougall D, et al. Expansion of the Lyme Disease Vector Ixodes Scapularis in Canada Inferred from CMIP5 Climate Projections. Environ Health Perspect. 2017;125(5):057008. doi: 10.1289/EHP57 28599266
17. Lempereur L, Beck R, Fonseca I, Marques C, Duarte A, Santos M, et al. Guidelines for the Detection of Babesia and Theileria Parasites. Vector Borne Zoonotic Dis. 2017;17(1):51–65. doi: 10.1089/vbz.2016.1955 28055573
18. Ord RL, Lobo CA. Human Babesiosis: Pathogens, Prevalence, Diagnosis and Treatment. Curr Clin Microbiol Rep. 2015;2(4):173–81. doi: 10.1007/s40588-015-0025-z 26594611
19. Usmani-Brown S, Halperin JJ, Krause PJ. Neurological manifestations of human babesiosis. Handb Clin Neurol. 2013;114:199–203. doi: 10.1016/B978-0-444-53490-3.00014-5 23829910
20. Gray JS. Identity of the causal agents of human babesiosis in Europe. Int J Med Microbiol. 2006;296 Suppl 40:131–6.
21. Gelfand JA, Callahan MV. Babesiosis: An Update on Epidemiology and Treatment. Curr Infect Dis Rep. 2003;5(1):53–8. doi: 10.1007/s11908-003-0065-z 12525291
22. Dunn IJ, Palmer PE. Babesiosis. Semin Roentgenol. 1998;33(1):89–90. doi: 10.1016/s0037-198x(98)80035-7 9516693
23. Spielman A, Wilson ML, Levine JF, Piesman J. Ecology of Ixodes dammini-borne human babesiosis and Lyme disease. Annu Rev Entomol. 1985;30:439–60. doi: 10.1146/annurev.en.30.010185.002255 3882050
24. Rosner F, Zarrabi MH, Benach JL, Habicht GS. Babesiosis in splenectomized adults. Review of 22 reported cases. Am J Med. 1984;76(4):696–701. doi: 10.1016/0002-9343(84)90298-5 6424470
25. Ruebush TK II. Human babesiosis in North America. Trans R Soc Trop Med Hyg. 1980;74(2):149–52. doi: 10.1016/0035-9203(80)90231-x 7189910
26. Open Grey [cited 20 August 2019]. http://www.opengrey.eu/.
27. DataCite [cited 20 August 2019]. https://search.datacite.org/.
28. Cayol C, Koskela E, Mappes T, Siukkola A, Kallio ER. Temporal dynamics of the tick Ixodes ricinus in northern Europe: epidemiological implications. Parasit Vectors. 2017;10(1):166. doi: 10.1186/s13071-017-2112-x 28359294
29. Goethert HK, Telford SR 3rd. Not "out of Nantucket": Babesia microti in southern New England comprises at least two major populations. Parasit Vectors. 2014;7:546. doi: 10.1186/s13071-014-0546-y 25492628
30. Lemieux JE, Tran AD, Freimark L, Schaffner SF, Goethert H, Andersen KG, et al. A global map of genetic diversity in Babesia microti reveals strong population structure and identifies variants associated with clinical relapse. Nat Microbiol. 2016;1(7):16079. doi: 10.1038/nmicrobiol.2016.79 27572973
31. Morch K, Holmaas G, Frolander PS, Kristoffersen EK. Severe human Babesia divergens infection in Norway. Int J Infect Dis. 2015;33:37–8. doi: 10.1016/j.ijid.2014.12.034 25541295
32. Gabrielli S, Galuppi R, Marcer F, Marini C, Tampieri MP, Moretti A, et al. Development of culture-based serological assays to diagnose Babesia divergens infections. Vector Borne Zoonotic Dis. 2012;12(2):106–10. doi: 10.1089/vbz.2011.0706 21995263
33. El-Bahnasawy MM, Khalil HH, Morsy TA. Babesiosis in an Egyptian boy aquired from pet dog, and a general review. J Egypt Soc Parasitol. 2011;41(1):99–108. 21634246
34. Gorenflot A, Piette M. Aspects microscopiques observés au cours des deux premiers cas français de Babésiose humaine. Med Mal Infect. 1981;11(6):334–8.
35. Apostolou A, Sorhage F, Tan C. Babesiosis surveillance, new jersey, USA, 2006–2011. Emerg Infect Dis. 2014;20(8):1407–9. doi: 10.3201/eid2008.131591 25062278
36. Surra ND, Jesus JE. The anemic and thrombocytopenic febrile neonate. J Emerg Med. 2015;48(6):675–8. doi: 10.1016/j.jemermed.2014.11.026 25895861
37. Joseph JT, Purtill K, Wong SJ, Munoz J, Teal A, Madison-Antenucci S, et al. Vertical transmission of Babesia microti, United States. Emerg Infect Dis. 2012;18(8):1318–21. doi: 10.3201/eid1808.110988 22840424
38. Aderinboye O, Syed SS. Congenital babesiosis in a four-week-old female infant. Pediatr Infect Dis J. 2010;29(2):188.
39. New DL, Quinn JB, Qureshi MZ, Sigler SJ. Vertically transmitted babesiosis. J Pediatr. 1997;131(1 Pt 1):163–4. doi: 10.1016/s0022-3476(97)70143-4 9255211
40. Esernio-Jenssen D, Scimeca PG, Benach JI, Tenenbaum MJ. Transplacental/perinatal babesiosis. Obstet Gynecol Surv. 1987;42(11):691–2.
41. Sethi S, Alcid D, Kesarwala H, Tolan RW Jr. Probable congenital babesiosis in infant, New Jersey, USA. Emerg Infect Dis. 2009;15(5):788–91. doi: 10.3201/eid1505.070808 19402971
42. Cornett JK, Malhotra A, Hart D. Vertical transmission of babesiosis from a pregnant, splenectomized mother to her neonate. Infect Dis Clin Pract (Baltim Md). 2012;20(6):408–10.
43. Saetre K, Godhwani N, Maria M, Patel D, Wang G, Li KI, et al. Congenital Babesiosis After Maternal Infection With Borrelia burgdorferi and Babesia microti. J Pediatric Infect Dis Soc. 2017;7:e1–e5.
44. Gumber S, Nascimento FS, Rogers KA, Bishop HS, Rivera HN, Xayavong MV, et al. Experimental transfusion-induced Babesia microti infection: dynamics of parasitemia and immune responses in a rhesus macaque model. Transfusion. 2016;56(6 Pt 2):1508–19. doi: 10.1111/trf.13521 26892459
45. Eberhard ML, Walker EM, Steurer FJ. Survival and infectivity of Babesia in blood maintained at 25 C and 2–4 C. J Parasitol. 1995;81(5):790–2. 7472878
46. Tufts DM, Diuk-Wasser MA. Transplacental transmission of tick-borne Babesia microti in its natural host Peromyscus leucopus. Parasit Vectors. 2018;11:286. doi: 10.1186/s13071-018-2875-8 29728129
47. Tolkacz K, Bednarska M, Alsarraf M, Dwuznik D, Grzybek M, Welc-Faleciak R, et al. Prevalence, genetic identity and vertical transmission of Babesia microti in three naturally infected species of vole, Microtus spp. (Cricetidae). Parasit Vectors. 2017;10(1):66. doi: 10.1186/s13071-017-2007-x 28166832
48. Bednarska M, Bajer A, Drozdowska A, Mierzejewska EJ, Tolkacz K, Welc-Faleciak R. Vertical Transmission of Babesia microti in BALB/c Mice: Preliminary Report. PLoS ONE. 2015;10(9):e0137731. doi: 10.1371/journal.pone.0137731 26372043
49. Nilsson O, Nordkvist M, Rydén L. Experimental Babesia divergens infection in reindeer (Rangifer tarandus). Acta Vet Scand. 1965;6(4):353–9. 5858323
50. Gray JS, Murphy TM, Taylor SM, Blewett DA, Harrington R. Comparative morphological and cross transmission studies with bovine and deer babesias in Ireland. Prev Vet Med. 1990;9(3):185–93.
51. Van Peenen PFD, Duncan HJF. Piroplasms (Protozoa: Sarcodina) of Wild Mammals in California 1. Bulletin of the Wildlife Disease Association. 1968;4(1):3–8.
52. Malagon F, Tapia JL. Experimental transmission of Babesia microti infection by the oral route. Parasitol Res. 1994;80(8):645–8. doi: 10.1007/bf00932947 7886033
53. Piesman J, Lewengrub S, Rudzinska MA, Spielman A. Babesia microti: prolonged survival of salavarian piroplasms in nymphal Ixodes dammini. Exp Parasitol. 1987;64(3):292–9. doi: 10.1016/0014-4894(87)90039-7 3678441
54. Karakashian SJ, Rudzinska MA, Spielman A, Lewengrub S, Piesman J, Shoukrey N. Ultrastructural studies on sporogony of Babesia microti in salivary gland cells of the tick Ixodes dammini. Cell Tissue Res. 1983;231(2):275–87. doi: 10.1007/bf00222180 6850804
55. Piesman J, Karakashian SJ, Lewengrub S. Development of Babesia microti sporozoites in adult Ixodes dammini. Int J Parasitol. 1986;16(4):381–5. doi: 10.1016/0020-7519(86)90118-9 3744675
56. Lewengrub S, Rudzinska MA, Piesman J, Spielman A, Zung J. The influence of heat on the development of Babesia microti in unfed nymphs of Ixodes dammini. Can J Zool. 1989;67(6):1510–5.
57. Lewengrub S, Rudzinska MA, Piesman J, Spielman A, Gubert E. Hyperthermia and sporogony of Babesia microti in the tick Ixodes dammini: an ultrastructural study. Can J Zool. 1988;66(6):1342–51.
58. Karakashian SJ, Rudzinska MA, Spielman A, Lewengrub S, Campbell J. Primary and secondary ookinetes of Babesia microti in the larval and nymphal stages of the tick Ixodes dammini. Can J Zool. 1986;64(2):328–39.
59. Bonnet S, Brisseau N, Hermouet A, Jouglin M, Chauvin A. Experimental in vitro transmission of Babesia sp. (EU1) by Ixodes ricinus. Vet Res. 2009;40(3):21. doi: 10.1051/vetres/2009004 19210953
60. Mackenstedt U, Gauer M, Mehlhorn H, Schein E, Hauschild S. Sexual cycle of Babesia divergens confirmed by DNA measurements. Parasitol Res. 1990;76(3):199–206. doi: 10.1007/bf00930815 2315280
61. Weber G, Walter G. Babesia microti (apicomplexa: piroplasmida): electron microscope detection in salivary glands of the tick vector Ixodes ricinus (Ixodoidea: Ixodidae). Z Parasitenkd. 1980;64(1):113–5. doi: 10.1007/bf00927061 7222920
62. Kuźna-Grygiel W, Bukowska K, Cichocka A, Kosik-Bogacka D, Skotarczak B. The prevalence of piroplasms in a population of Ixodes ricinus (ACARI: Ixodidae) from North-Western Poland. Ann Agric Environ Med. 2002;9(2):175–8. 12498586
63. Zamoto-Niikura A, Tsuji M, Qiang W, Nakao M, Hirata H, Ishihara C. Detection of two zoonotic Babesia microti lineages, the Hobetsu and U.S. lineages, in two sympatric tick species, ixodes ovatus and Ixodes persulcatus, respectively, in Japan. Appl Environ Microbiol. 2012;78(9):3424–30. doi: 10.1128/AEM.00142-12 22389378
64. Rudzinska M, Spielman A, Lewengrub S, Piesman J, Karakashian S. The sequence of developmental events of Babesia microti in the gut of Ixodes dammini. Protistologica. 1984;20(4):649–63.
65. Rudzinska M, Spielman A, Riek RF, Lewengrub SJ, Piesman J. Intraerythrocytic ‘gametocytes’ of Babesia microti and their maturation in ticks. Can J Zool. 1979;57(2):424–34. doi: 10.1139/z79-050 540277
66. Rudzinska MA, Spielman A, Lewengrub S. Penetration of the peritrophic membrane of the tick by Babesia microti. Cell Tissue Res. 1981;221(3):471–81.
67. Farber FR, Muehlenbachs A, Robey TE. Atraumatic splenic rupture from Babesia: A disease of the otherwise healthy patient. Ticks Tick Borne Dis. 2015;6(5):649–52. doi: 10.1016/j.ttbdis.2015.05.010 26123434
68. Kuwayama DP, Briones RJ. Spontaneous splenic rupture caused by Babesia microti infection. Clin Infect Dis. 2008;46(9):e92–5. doi: 10.1086/587175 18419430
69. Torres-Velez FJ, Nace EK, Won KY, Bartlett J, Eberhard M, Guarner J. Development of an immunohistochemical assay for the detection of babesiosis in formalin-fixed, paraffin-embedded tissue samples. Am J Clin Pathol. 2003;120(6):833–8. doi: 10.1309/A4RG-P4LF-12GG-H8MW 14671971
70. Siderits R, Mikhail N, Ricart C, Abello-Poblete MV, Wilcox C, Godyn JJ. Babesiosis, significance of spleen function illustrated by postsplenectomy course in 3 cases. Infect Dis Clin Pract (Baltim Md). 2008;16(3):182–6.
71. Brennan MB, Herwaldt BL, Kazmierczak JJ, Weiss JW, Klein CL, Leith CP, et al. Transmission of Babesia microti Parasites by Solid Organ Transplantation. Emerg Infect Dis. 2016;22(11):1869–76.
72. Akel T, Mobarakai N. Hematologic manifestations of babesiosis. Ann Clin Microbiol Antimicrob. 2017;16(1):6. doi: 10.1186/s12941-017-0179-z 28202022
73. Man SQ, Qiao K, Cui J, Feng M, Fu YF, Cheng XJ. A case of human infection with a novel Babesia species in China. Infect Dis Poverty. 2016;5:28. doi: 10.1186/s40249-016-0121-1 27025290
74. Andric B, Golubovic M, Terzic D, Dupanovic B, Icevic M. First diagnostic cases of human babesiosis in Montenegro. Braz J Infect Dis. 2012;16(5):498–9. doi: 10.1016/j.bjid.2012.04.001 22975172
75. Javed MZ, Srivastava M, Zhang S, Kandathil M. Concurrent babesiosis and ehrlichiosis in an elderly host. Mayo Clin Proc. 2001;76(5):563–5. doi: 10.4065/76.5.563 11357805
76. Slovut DP, Benedetti E, Matas AJ. Babesiosis and hemophagocytic syndrome in an asplenic renal transplant recipient. Transplantation. 1996;62(4):537–9. doi: 10.1097/00007890-199608270-00018 8781622
77. Auerbach M, Haubenstock A, Soloman G. Systemic babesiosis. Another cause of the hemophagocytic syndrome. Am J Med. 1986;80(2):301–3. doi: 10.1016/0002-9343(86)90028-8 3946448
78. Ortiz JM, Eagle RC Jr. Ocular findings in human babesiosis (nantucket fever). Am J Ophthalmol. 1982;93(3):307–11. doi: 10.1016/0002-9394(82)90530-x 7200325
79. Acosta MEP, Ender PT, Smith EM, Jahre JA. Babesia microti infection, eastern Pennsylvania, USA. Emerg Infect Dis. 2013;19(7):1105–7. doi: 10.3201/eid1907.121593 23764008
80. Scharfman WB. Nantucket fever. An additional case of babesiosis. J Am Med Assoc. 1977;238(12):1281–2.
81. Blackberg J, Lazarevic VL, Hunfeld KP, Persson KEM. Low-virulent Babesia venatorum infection masquerading as hemophagocytic syndrome. Ann Hematol. 2017;97:731–3. doi: 10.1007/s00277-017-3220-6 29285582
82. Narurkar R, Mamorska-Dyga A, Nelson JC, Liu D. Autoimmune hemolytic anemia associated with babesiosis. Biomark Res. 2017;5:14. doi: 10.1186/s40364-017-0095-6 28405337
83. Feliberti JP, Iyer D, Mody K, Almendral J. An unusual case of anemia in a heart transplant patient. J Am Coll Cardiol. 2017;69 (11):2386.
84. Jablonska J, Zarnowska-Prymek H, Stanczak J, Kozlowska J, Wiercinska-Drapalo A. Symptomatic co-infection with Babesia microti and Borrelia burgdorferi in patient after international exposure; a challenging case in Poland Ann Agric Environ Med. 2016;23(2):387–9. doi: 10.5604/12321966.1203914 27294655
85. Moniuszko-Malinowska A, Swiecicka I, Dunaj J, Zajkowska J, Czupryna P, Zambrowski G, et al. Infection with Babesia microti in humans with non-specific symptoms in North East Poland. Infect Dis (Lond). 2016;48(7):537–43.
86. Tomasiewicz K, Chmielewska-Badora J, Zwolinski J, Murias-Brylowska E. Analysis of main T-cell subsets and activated T supressor/cytotoxic cells in patients with Borrelia burgdorferi s. lato only infection and co-infections with Anaplasma phagocytophilum, Bartonella spp. and Babesia microti. Ann Agric Environ Med. 2016;23(1):111–5. doi: 10.5604/12321966.1196864 27007527
87. Surgers L, Belkadi G, Foucard A, Lalande V, Girard PM, Hennequin C. Babesiosis and Lyme disease co-infection in a female patient returning from the United States. Med Mal Infect. 2015;45(11–12):490–2. doi: 10.1016/j.medmal.2015.10.002 26525187
88. Mayne PJ. Clinical determinants of Lyme borreliosis, babesiosis, bartonellosis, anaplasmosis, and ehrlichiosis in an Australian cohort. Int J Gen Med. 2014;8:15–26. doi: 10.2147/IJGM.S75825 25565883
89. Opalinska P, Wierzbicka A, Asman M. The PCR and nested PCR detection of Borrelia burgdorferi sensu lato, Anaplasma phagocytophilum and Babesia microti in Dermacentor reticulatus F. collected in a new location in Poland (Trzciel, Western Poland). Acta Parasitol. 2016;61(4):849–54. doi: 10.1515/ap-2016-0117 27787203
90. Mierzejewska EJ, Pawelczyk A, Radkowski M, Welc-Faleciak R, Bajer A. Pathogens vectored by the tick, Dermacentor reticulatus, in endemic regions and zones of expansion in Poland. Parasit Vectors. 2015;8:490. doi: 10.1186/s13071-015-1099-4 26403456
91. Wojcik-Fatla A, Zajac V, Sawczyn A, Cisak E, Dutkiewicz J. Babesia spp. in questing ticks from eastern Poland: prevalence and species diversity. Parasitol Res. 2015;114(8):3111–6. doi: 10.1007/s00436-015-4529-5 25976982
92. Wojcik-Fatla A, Bartosik K, Buczek A, Dutkiewicz J. Babesia microti in adult Dermacentor reticulatus ticks from eastern Poland. Vector Borne Zoonotic Dis. 2012;12(10):841–3. doi: 10.1089/vbz.2011.0904 22651392
93. Garcia-Sanmartin J, Barandika JF, Juste RA, Garcia-Perez AL, Hurtado A. Distribution and molecular detection of Theileria and Babesia in questing ticks from northern Spain. Med Vet Entomol. 2008;22(4):318–25. doi: 10.1111/j.1365-2915.2008.00748.x 19120958
94. Welc-Faleciak R, Bajer A, Behnke JM, Sinski E. Effects of host diversity and the community composition of hard ticks (Ixodidae) on Babesia microti infection. Int J Med Microbiol. 2008;298(Suppl. 1):235–42.
95. Radzijevskaja J, Mardosaite-Busaitiene D, Aleksandraviciene A, Paulauskas A. Investigation of Babesia spp. in sympatric populations of Dermacentor reticulatus and Ixodes ricinus ticks in Lithuania and Latvia. Ticks Tick Borne Dis. 2017;9:270–4. doi: 10.1016/j.ttbdis.2017.09.013 28969995
96. Zajac V, Wojcik-Fatla A, Sawczyn A, Cisak E, Sroka J, Kloc A, et al. Prevalence of infections and co-infections with 6 pathogens in Dermacentor reticulatus ticks collected in eastern Poland. Ann Agric Environ Med. 2017;24:26–32. doi: 10.5604/12321966.1233893 28378977
97. Michelet L, Joncour G, Devillers E, Torina A, Vayssier-Taussat M, Bonnet SI, et al. Tick species, tick-borne pathogens and symbionts in an insular environment off the coast of Western France. Ticks Tick Borne Dis. 2016;7(6):1109–15. doi: 10.1016/j.ttbdis.2016.08.014 27622976
98. Hilpertshauser H, Deplazes P, Schnyder M, Gern L, Mathis A. Babesia spp. identified by PCR in ticks collected from domestic and wild ruminants in southern Switzerland. Appl Environ Microbiol. 2006;72(10):6503–7. doi: 10.1128/AEM.00823-06 17021198
99. Oksana K, Natalia S, Andrei P, Alexandr M, Inga U, Ion T. Mono- and Mixed- infections of tick-borne pathogens in various ecological foci in Moldova. Buletinul Academiei de Ştiinţe a Moldovei Ştiinţele vieţii. 2016;3:122–6.
100. Jia N, Zheng YC, Jiang JF, Jiang RR, Jiang BG, Wei R, et al. Human Babesiosis Caused by a Babesia crassa-like Pathogen: A Case Series. Clin Infect Dis. 2018;67(6):1110–9.
101. Zhang H, Sun Y, Jiang H, Huo X. Prevalence of Severe Febrile and Thrombocytopenic Syndrome Virus, Anaplasma spp. and Babesia microti in Hard Ticks (Acari: Ixodidae) from Jiaodong Peninsula, Shandong Province. Vector Borne Zoonotic Dis. 2017;17(2):134–40. doi: 10.1089/vbz.2016.1978 28048951
102. Wei F, Song M, Liu H, Wang B, Wang S, Wang Z, et al. Molecular Detection and Characterization of Zoonotic and Veterinary Pathogens in Ticks from Northeastern China. Front Microbiol. 2016;7:1913. doi: 10.3389/fmicb.2016.01913 27965644
103. Chen Z, Liu Q, Liu J, Xu B, Lv S, Xia S, et al. Tick-borne pathogens and associated co-infections in ticks collected from domestic animals in central China. Parasit Vectors. 2014;7:237. doi: 10.1186/1756-3305-7-237 24886497
104. Morozov AC, Tischenkov AA, Proka AA, Silaghi C, Toderas IK, Movila AA, et al. Prevalence of tick-borne pathogens in ticks from migratory birds in republic of Moldova. Parasit Vectors. 2014;7(Suppl 1):P4.
105. Rybarova M, Honsova M, Papousek I, Siroky P. Variability of species of Babesia Starcovici, 1893 in three sympatric ticks (Ixodes ricinus, Dermacentor reticulatus and Haemaphysalis concinna) at the edge of Pannonia in the Czech Republic and Slovakia. Folia Parasitol (Praha). 2017;64.
106. Hamsikova Z, Kazimirova M, Harustiakova D, Mahrikova L, Slovak M, Berthova L, et al. Babesia spp. in ticks and wildlife in different habitat types of Slovakia. Parasit Vectors. 2016;9(1):292. doi: 10.1186/s13071-016-1560-z 27207099
107. Goethert HK, Telford SR Iii. Enzootic transmission of Babesia divergens among cottontail rabbits on Nantucket Island, Massachusetts. Am J Trop Med Hyg. 2003;69(5):455–60. 14695079
108. Rar VA, Epikhina TI, Livanova NN, Panov VV, Pukhovskaya NM, Vysochina NP, et al. Detection of Babesia DNA in small mammals and ixodid ticks in the North Urals, Western Siberia, and Far East of Russia. Mol Gen Microbiol Virol. 2010;25(3):118–23.
109. Chaligiannis I, Fernandez de Mera IG, Papa A, Sotiraki S, de la Fuente J. Molecular identification of tick-borne pathogens in ticks collected from dogs and small ruminants from Greece. Exp Appl Acarol. 2018;74:443–53. doi: 10.1007/s10493-018-0237-z 29516380
110. Cassini R, Marcer F, di Regalbono AF, Cancrini G, Gabrielli S, Moretti A, et al. New insights into the epidemiology of bovine piroplasmoses in Italy. Vet Parasitol. 2012;184(1):77–82. doi: 10.1016/j.vetpar.2011.08.004 21864982
111. Karasartova D, Gureser AS, Gokce T, Celebi B, Yapar D, Keskin A, et al. Bacterial and protozoal pathogens found in ticks collected from humans in Corum province of Turkey. PLoS Negl Trop Dis. 2018;12:e0006395. doi: 10.1371/journal.pntd.0006395 29649265
112. Ogo NI, de Mera IG, Galindo RC, Okubanjo OO, Inuwa HM, Agbede RI, et al. Molecular identification of tick-borne pathogens in Nigerian ticks. Vet Parasitol. 2012;187(3–4):572–7. doi: 10.1016/j.vetpar.2012.01.029 22326937
113. Lv J, Fernandez de Marco MDM, Goharriz H, Phipps LP, McElhinney LM, Hernandez-Triana LM, et al. Detection of tick-borne bacteria and babesia with zoonotic potential in Argas (Carios) vespertilionis (Latreille, 1802) ticks from British bats. Sci Rep. 2018;8:1865. doi: 10.1038/s41598-018-20138-1 29382871
114. Maamun JM, Suleman MA, Akinyi M, Ozwara H, Kariuki T, Carlsson HE. Prevalence of Babesia microti in free-ranging baboons and African green monkeys. J Parasitol. 2011;97(1):63–7. doi: 10.1645/GE-2391.1 21348608
115. Mancini F, Di Luca M, Toma L, Vescio F, Bianchi R, Khoury C, et al. Prevalence of tick-borne pathogens in an urban park in Rome, Italy. Ann Agric Environ Med. 2014;21(4):723–7. doi: 10.5604/12321966.1129922 25528909
116. Georges K, Loria GR, Riili S, Greco A, Caracappa S, Jongejan F, et al. Detection of haemoparasites in cattle by reverse line blot hybridisation with a note on the distribution of ticks in Sicily. Vet Parasitol. 2001;99(4):273–86. doi: 10.1016/s0304-4017(01)00488-5 11511414
117. Pietrobelli M, Cancrini G, Moretti A, Tampieri MP. Animal babesiosis: an emerging zoonosis also in Italy? Parassitologia. 2007;49 Suppl 1:33–8.
118. Rudolf I, Golovchenko M, Šikutová S, Rudenko N, Grubhoffer L, Hubálek Z. Babesia microti (Piroplasmida: Babesiidae) in nymphal Ixodes ricinus (Acari: Ixodidae) in the Czech Republic. Folia Parasitol (Praha). 2005;52(3):274–6.
119. Katargina O, Geller J, Vasilenko V, Kuznetsova T, Jarvekulg L, Vene S, et al. Detection and characterization of Babesia species in Ixodes ticks in Estonia. Vector Borne Zoonotic Dis. 2011;11(7):923–8. doi: 10.1089/vbz.2010.0199 21395407
120. Mrljak V, Rafaj RB, Sušić V, Matijatko V, Kučer N, Kiš I. Antithrombin III in healthy dogs and in dogs suffering from babesiosis. Veterinarski Arhiv. 2005;75(6):477–86.
121. Health M. Manitoba annual tick-borne disease report, 2016. 2017 Contract No.: Report.
122. Burkot TR, Maupin GO, Schneider BS, Denatale C, Happ CM, Rutherford JS, et al. Use of a sentinel host system to study the questing behavior of Ixodes spinipalpis and its role in the transmission of Borrelia bissettii, human granulocytic ehrlichiosis, and Babesia microti. Am J Trop Med Hyg. 2001;65(4):293–9. doi: 10.4269/ajtmh.2001.65.293 11693872
123. Stafford KC III, Williams SC, Magnarelli LA, Bharadwaj A, Ertel SH, Nelson RS. Expansion of zoonotic babesiosis and reported human cases, Connecticut, 2001–2010. J Med Entomol. 2014;51(1):245–52. doi: 10.1603/me13154 24605475
124. Da Rold G, Ravagnan S, Soppelsa F, Porcellato E, Soppelsa M, Obber F, et al. Ticks are more suitable than red foxes for monitoring zoonotic tick-borne pathogens in northeastern Italy. Parasit Vectors. 2018;11:137. doi: 10.1186/s13071-018-2726-7 29554970
125. Hornok S, Szoke K, Kovats D, Estok P, Gorfol T, Boldogh SA, et al. DNA of Piroplasms of Ruminants and Dogs in Ixodid Bat Ticks PLoS ONE. 2016;11(12):e0167735. doi: 10.1371/journal.pone.0167735 27930692
126. Herwaldt BL, Linden JV, Bosserman E, Young C, Olkowska D, Wilson M. Transfusion-associated babesiosis in the United States: a description of cases. Ann Intern Med. 2011;155(8):509–19. doi: 10.7326/0003-4819-155-8-201110180-00362 21893613
127. Xu G, Mather TN, Hollingsworth CS, Rich SM. Passive Surveillance of Ixodes scapularis (Say), Their Biting Activity, and Associated Pathogens in Massachusetts Vector Borne Zoonotic Dis. 2016;16(8):520–7. doi: 10.1089/vbz.2015.1912 27248292
128. Stromdahl E, Hamer S, Jenkins S, Sloan L, Williamson P, Foster E, et al. Comparison of phenology and pathogen prevalence, including infection with the Ehrlichia muris-like (EML) agent, of Ixodes scapularis removed from soldiers in the midwestern and the northeastern United States over a 15 year period (1997–2012). Parasit Vectors. 2014;7:553. doi: 10.1186/s13071-014-0553-z 25465046
129. O’Brien SF, Delage G, Scalia V, Lindsay R, Bernier F, Dubuc S, et al. Seroprevalence of Babesia microti infection in Canadian blood donors. Transfusion. 2016;56(1):237–43. doi: 10.1111/trf.13339 26426217
130. Shoemaker RC, Hudnell HK, House DE, Kempen A, Pakes GE. Atovaquone plus cholestyramine in patients coinfected with Babesia microti and Borrelia burgdorferi refractory to other treatment. Adv Ther. 2006;23(1):1–11. doi: 10.1007/bf02850341 16644602
131. Farzad E, Cator M, Giulivi A, Zhang J. Physician survey on knowledge and reporting practices of transfusion-transmitted infections in Canada Can J Public Health. 2004;95(6):451–5. 15622796
132. Guerrero Espejo A, Munoz Parada C, Tomas Dols S. Incidence of human babesiosis in Spain obtained from the diagnoses at hospital discharge. Med Clin (Barc). 2017;149:84–5.
133. Connally NP, Hinckley AF, Feldman KA, Kemperman M, Neitzel D, Wee SB, et al. Testing practices and volume of non-Lyme tickborne diseases in the United States. Ticks Tick Borne Dis. 2016;7(1):193–8. doi: 10.1016/j.ttbdis.2015.10.005 26565931
134. Capelli G, Ravagnan S, Montarsi F, Ciocchetta S, Cazzin S, Porcellato E, et al. Occurrence and identification of risk areas of Ixodes ricinus-borne pathogens: a cost-effectiveness analysis in north-eastern Italy. Parasit Vectors. 2012;5:61. doi: 10.1186/1756-3305-5-61 22452970
135. Bish EK, Moritz ED, El-Amine H, Bish DR, Stramer SL. Cost-effectiveness of Babesia microti antibody and nucleic acid blood donation screening using results from prospective investigational studies. Transfusion. 2015;55(9):2256–71. doi: 10.1111/trf.13136 25995054
136. Goodell AJ, Bloch EM, Krause PJ, Custer B. Costs, consequences, and cost-effectiveness of strategies for Babesia microti donor screening of the US blood supply. Transfusion. 2014;54(9):2245–57. doi: 10.1111/trf.12805 25109338
137. Simon MS, Leff JA, Pandya A, Cushing M, Shaz BH, Calfee DP, et al. Cost-effectiveness of blood donor screening for Babesia microti in endemic regions of the United States. Transfusion. 2013;54(3 Pt 2):889–99. doi: 10.1111/trf.12492 24252132
138. McCullough J, Goldfinger D, Gorlin J, Riley WJ, Sandhu H, Stowell C, et al. Cost implications of implementation of pathogen-inactivated platelets. Transfusion. 2015;55(10):2312–20. doi: 10.1111/trf.13149 25989465
139. Kim J, Cho S, Joo H, Tsuji M, Cho S, Park I, et al. First case of human babesiosis in Korea: detection and characterization of a novel type of Babesia sp. (KO1) similar to ovine Babesia. J Clin Microbiol. 2007;45(6):2084–7. doi: 10.1128/JCM.01334-06 17392446
140. Wilson M, Glaser KC, Adams-Fish D, Boley M, Mayda M, Molestina RE. Development of droplet digital PCR for the detection of Babesia microti and Babesia duncani. Exp Parasitol. 2015;149:24–31. doi: 10.1016/j.exppara.2014.12.003 25500215
141. Magnarelli LA, Dumler JS, Anderson JF, Johnson RC, Fikrig E. Coexistence of antibodies to tick-borne pathogens of babesiosis, ehrlichiosis, and Lyme borreliosis in human sera. J Clin Microbiol. 1995;33(11):3054–7. 8576376
142. Krause PJ, Telford SR 3rd, Spielman A, Sikand V, Ryan R, Christianson D, et al. Concurrent Lyme disease and babesiosis. Evidence for increased severity and duration of illness. JAMA. 1996;275(21):1657–60. 8637139
143. Krause PJ, McKay K, Thompson CA, Sikand VK, Lentz R, Lepore T, et al. Disease-specific diagnosis of coinfecting tickborne zoonoses: babesiosis, human granulocytic ehrlichiosis, and Lyme disease. Clin Infect Dis. 2002;34(9):1184–91. doi: 10.1086/339813 11941544
144. Vannier EG, Diuk-Wasser MA, Ben Mamoun C, Krause PJ. Babesiosis. Infect Dis Clin North Am. 2015;29(2):357–70. doi: 10.1016/j.idc.2015.02.008 25999229
145. Krause PJ, Gewurz BE, Hill D, Marty FM, Vannier E, Foppa IM, et al. Persistent and relapsing babesiosis in immunocompromised patients. Clinical Infectious Diseases. 2008;46(3):370–6. doi: 10.1086/525852 18181735
146. Mareedu N, Schotthoefer AM, Tompkins J, Hall MC, Fritsche TR, Frost HM. Risk Factors for Severe Infection, Hospitalization, and Prolonged Antimicrobial Therapy in Patients with Babesiosis. Am J Trop Med Hyg. 2017;97:1218–25. doi: 10.4269/ajtmh.17-0146 28722598
147. Spaete J, Patrozou E, Rich JD, Sweeney JD. Red cell exchange transfusion for babesiosis in Rhode Island. J Clin Apher. 2009;24(3):97–105. doi: 10.1002/jca.20197 19291782
148. Zintl A, Mulcahy G, Skerrett HE, Taylor SM, Gray JS. Babesia divergens, a bovine blood parasite of veterinary and zoonotic importance. Clin Microbiol Rev. 2003;16(4):622–36. doi: 10.1128/CMR.16.4.622-636.2003 14557289
149. Wormser GP, Prasad A, Neuhaus E, Joshi S, Nowakowski J, Nelson J, et al. Emergence of resistance to azithromycin-atovaquone in immunocompromised patients with Babesia microti infection. Clin Infect Dis. 2010;50(3):381–6. doi: 10.1086/649859 20047477
150. Scott JD. First record of locally acquired human babesiosis in Canada caused by Babesia duncani: a case report. SAGE Open Med Case Rep. 2017;5:2050313X17725645.
151. Bullard JM, Ahsanuddin AN, Perry AM, Lindsay LR, Iranpour M, Dibernardo A, et al. The first case of locally acquired tick-borne Babesia microti infection in Canada. Can J Infect Dis Med Microbiol. 2014;25(6):e87–9. doi: 10.1155/2014/209521 25587297
152. Warren T, Lau R, Ralevski F, Rau N, Boggild AK. Fever in a visitor to Canada: a case of mistaken identity. J Clin Microbiol. 2015;53(5):1783–5. doi: 10.1128/JCM.00269-15 25762775
153. dos Santos CC, Kain KC. Two tick-borne diseases in one: a case report of concurrent babesiosis and Lyme disease in Ontario. CMAJ. 1999;160(13):1851–3. 10405671
154. Kunimoto D, Krause K, Morrison D. First case of (imported) babesiosis diagnosed in Canada Can J Infect Dis. 1998;9(6):387–9. doi: 10.1155/1998/564190 22346559
155. Cd Santos, Kain K. Concurrent babesiosis and Lyme disease diagnosed in Ontario Can Commun Dis Rep. 1998;24(12):97–101. 9659788
156. Jassoum SB, Fong IW, Hannach B, Kain KC. Transfusion-transmitted babesiosis in Ontario: first reported case in Canada. Can Commun Dis Rep. 2000;26(2):9–13. 10680253
157. Filstein MR, Benach JL, White DJ, Brody BA, Goldman WD, Bakal CW, et al. Serosurvey for human babesiosis in New York. J Infect Dis. 1980;141(4):518–21. doi: 10.1093/infdis/141.4.518 7189538
158. Krause PJ, Telford SR Iii, Ryan R, Hurta AB, Kwasnik I, Luger S, et al. Geographical and temporal distribution of babesial infection in Connecticut. J Clin Microbiol. 1991;29(1):1–4. 1993742
159. Brasseur P, Gorenflot A. Human babesiosis in Europe. Mem Inst Oswaldo Cruz. 1992;87 Suppl 3:131–2.
160. Fang DC, McCullough J. Transfusion-Transmitted Babesia microti. Transfus Med Rev. 2016;30(3):132–8. doi: 10.1016/j.tmrv.2016.04.002 27260107
161. Walsh GM, Shih AW, Solh Z, Golder M, Schubert P, Fearon M, et al. Blood-Borne Pathogens: A Canadian Blood Services Centre for Innovation Symposium. Transfus Med Rev. 2016;30(2):53–68. doi: 10.1016/j.tmrv.2016.02.003 26962008
162. Canadian Blood Services. Babesiosis Study 2018 [cited 23 May 2019]. https://blood.ca/en/blood/blood-safety/babesiosis-study-2018.
163. Lindsay LR, Ogden NH, Schofield SW. Review of methods to prevent and reduce the risk of Lyme disease. Can Commun Dis Rep. 2015;41(6):146–53. doi: 10.14745/ccdr.v41i06a04 29769946
164. Spielman A, Clifford CM, Piesman J, Corwin MD. Human babesiosis on Nantucket Island, USA: description of the vector, Ixodes (Ixodes) dammini, n. sp. (Acarina: Ixodidae). J Med Entomol. 1979;15(3):218–34. doi: 10.1093/jmedent/15.3.218 439119
165. Yabsley MJ, Shock BC. Natural history of Zoonotic Babesia: Role of wildlife reservoirs. Int J Parasitol Parasites Wildl. 2013;2:18–31. doi: 10.1016/j.ijppaw.2012.11.003 24533312
166. Marjolet M. Note to the editor. Bulletin de la Societe de Pathologie Exotique. 2002;95(4):304.
167. Swei A, O’Connor KE, Couper LI, Thekkiniath J, Conrad PA, Padgett KA, et al. Evidence for transmission of the zoonotic apicomplexan parasite Babesia duncani by the tick Dermacentor albipictus. Int J Parasitol. 2019;49(2):95–103. doi: 10.1016/j.ijpara.2018.07.002 30367862
Článek vyšel v časopise
PLOS One
2019 Číslo 12
- Proč se v Česku šíří několik „vymýcených“ infekcí najednou? Ptáme se odborníků
- ADHD jako evoluční výhoda? Výzkum se zaměřil na lovce a sběrače
- Není migréna jako migréna: Co pociťují ženy a co muži?
- Metamizol jako analgetikum první volby: kdy, pro koho, jak a proč?
- Není statin jako statin aneb praktický přehled rozdílů jednotlivých molekul
Nejčtenější v tomto čísle
- Methylsulfonylmethane increases osteogenesis and regulates the mineralization of the matrix by transglutaminase 2 in SHED cells
- Oregano powder reduces Streptococcus and increases SCFA concentration in a mixed bacterial culture assay
- Parametric CAD modeling for open source scientific hardware: Comparing OpenSCAD and FreeCAD Python scripts
- The characteristic of patulous eustachian tube patients diagnosed by the JOS diagnostic criteria