DOCSLIB.ORG

Case Definitions for Select Reportable Diseases in Florida Florida Department of Health Bureau of Epidemiology

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Case Definitions for Select Reportable Diseases in Florida Florida Department of Health Bureau of Epidemiology DRAFT Version1.4 Surveillance Case Definitions for Select Reportable Diseases in Florida Florida Department of Health Bureau of Epidemiology Department of Health Bureau of Epidemiology 4052 Bald Cypress Way, Bin A-12 Tallahassee, FL 32399-1720 Fax 850-922-9299 Confidential Fax 850-414-6894 850-245-4401 (24 hours/7 days) January 2010 DRAFT Version1.4 Contents INTRODUCTION.......................................................................................................... 1 List of Sterile and Non-Sterile Sites.......................................................................... 2 Suspect Immediately: Report immediately, 24 hours a day, 7 days a week (24/7), by phone upon initial clinical suspicion or laboratory test order............... 2 Immediately: Report immediately 24 hours a day, 7 days a week (24/7), by phone upon diagnosis............................................................................................... 2 Isolates or specimens are required to be submitted to the Bureau of Laboratories as required by Chapter 64D-3 Florida Administrative Code ......... 2 HOW TO USE INFORMATION IN THIS REPORT ...................................................... 2 Acute Arboviral Diseases (neuroinvasive and non-neuroinvasive)....................... 3 reporting code = 06210 Western Equine Encephalitis virus (neuroinvasive) = 06211 Western Equine Encephalitis virus (non-neuroinvasive) = 06220 Eastern Equine Encephalitis virus (neuroinvasive) = 06221 Eastern Equine Encephalitis virus (non-neuroinvasive) = 06230 St. Louis Encephalitis virus (neuroinvasive) = 06231 St. Louis Encephalitis virus (non-neuroinvasive) = 06250 California serogroup virus (neuroinvasive) = 06251 California serogroup virus (non-neuroinvasive) = 06620 Venezuelan Equine Encephalitis virus (neuroinvasive) = 06621 Venezuelan Equine Encephalitis virus (non-neuroinvasive) = 06630 West Nile virus (neuroinvasive) = 06631 West Nile virus (non-neuroinvasive) Amebic Encephalitis (Naegleria fowleri, Balamuthia mandrillaris, Acanthamoeba excluding A. keratitis)................................................................................................ 6 Anaplasmosis/Ehrlichiosis, Human (see Ehlirchiosis)........................................... 8 Anthrax........................................................................................................................9 Arsenic Poisoning.................................................................................................... 11 Botulism.................................................................................................................... 12 Brucellosis................................................................................................................ 13 Campylobacteriosis ................................................................................................. 14 Carbon Monoxide Poisoning................................................................................... 15 Cholera, Vibrio.......................................................................................................... 17 i DRAFT Version1.4 Ciguatera Poisoning ................................................................................................ 18 Creutzfeldt-Jakob Disease (CJD)............................................................................ 19 Cryptosporidiosis .................................................................................................... 20 Cyclosporiasis.......................................................................................................... 21 Dengue Fever ........................................................................................................... 22 Diphtheria .................................................................................................................. 24 Ehrlichiosis/Anaplasmosis, Human........................................................................ 25 Encephalitis, Other (Non-arboviral)........................................................................ 27 Escherichia coli, Shiga Toxin Producing (STEC) .................................................. 28 Giardiasis.................................................................................................................. 29 Glanders (Burkholderia mallei) .............................................................................. 30 Haemophilus influenzae (Invasive Disease) .......................................................... 31 Hansen’s Disease (Leprosy) ................................................................................... 32 Hantavirus Infection (Hantavirus Pulmonary Syndrome) ..................................... 33 Hemolytic Uremic Syndrome (HUS)........................................................................ 34 Hepatitis A ................................................................................................................ 35 Hepatitis B, Acute .................................................................................................... 36 Hepatitis B, Chronic................................................................................................. 37 Hepatitis B Surface Antigen (HBsAg+), in Pregnant Women ............................... 38 Hepatitis B, Perinatal ............................................................................................... 39 Hepatitis C, Acute .................................................................................................... 40 Hepatitis C, (Past or Present Infection).................................................................. 41 Hepatitis D ................................................................................................................ 42 Hepatitis E................................................................................................................. 43 Hepatitis G ................................................................................................................ 44 Influenza A, Novel or Pandemic Strains................................................................. 45 Influenza-Associated Pediatric Mortality ............................................................... 47 Lead Poisoning ........................................................................................................ 48 Legionellosis ............................................................................................................ 49 Leptospirosis............................................................................................................ 50 Listeriosis ................................................................................................................. 51 Lyme Disease ........................................................................................................... 52 ii DRAFT Version1.4 Malaria....................................................................................................................... 56 Measles (Rubeola).................................................................................................... 58 Melioidosis (Burkholderia pseudomallei) .............................................................. 60 Meningitis, Bacterial, Cryptococcal, Mycotic ........................................................ 61 Meningococcal Disease........................................................................................... 62 Mercury Poisoning................................................................................................... 63 Mumps....................................................................................................................... 64 Neurotoxic Shellfish Poisoning .............................................................................. 66 Pertussis................................................................................................................... 67 Pesticide-Related Illness and Injury ....................................................................... 68 Plague ....................................................................................................................... 71 Poliomyelitis, Paralytic ............................................................................................ 72 Poliomyelitis, Nonparalytic ..................................................................................... 72 Psittacosis ................................................................................................................ 74 Q Fever, Acute (Coxiella burnetii)........................................................................... 75 Q Fever, Chronic (Coxiella burnetii) ....................................................................... 76 Rabies, Animal ......................................................................................................... 78 Rabies, Human ......................................................................................................... 78 Rabies, Possible Exposure ..................................................................................... 79 Ricin Toxicity............................................................................................................ 80 Rocky Mountain Spotted Fever............................................................................... 81 Rubella ...................................................................................................................... 83 Rubella, Congenital Syndrome ..............................................................................
Load more

Recommended publications
  • LYME DISEASE Other Names: Borrelia Burgdorferi
    LYME DISEASE Other names: Borrelia burgdorferi CAUSE Lyme disease is caused by a spirochete bacteria (Borrelia burgdorferi) that is transmitted through the bite from an infected arthropod vector, the black-legged or deer tick Ixodes( scapularis). SIGNIFICANCE Lyme disease can infect people and some species of domestic animals (cats, dogs, horses, and cattle) causing mild to severe illness. Although wildlife can be infected by the bacteria, it typically does not cause illness in them. TRANSMISSION The bacteria has been observed in the blood of a number of wildlife species including several bird species but rarely appears to cause illness in these species. White-footed mice, eastern chipmunks, and shrews serve as the primary natural reservoirs for Lyme disease in eastern and central parts of North America. Other species appear to have low competencies as reservoirs for the bacteria. The transmission of Lyme disease is relatively convoluted due to the complex life cycle of the black-legged tick. This tick has multiple developmental stages and requires three hosts during its life cycle. The life cycle begins with the eggs of the ticks that are laid in the spring and from which larval ticks emerge. Larval ticks do not initially carryBorrelia burgdorferi, the bacteria must be acquired from their hosts they feed upon that are carriers of the bacteria. Through the summer the larval ticks feed on the blood of their first host, typically small mammals and birds. It is at this point where ticks may first acquireBorrelia burgdorferi. In the fall the larval ticks develop into nymphs and hibernate through the winter.
    [Show full text]
  • Phagocytosis of Borrelia Burgdorferi, the Lyme Disease Spirochete, Potentiates Innate Immune Activation and Induces Apoptosis in Human Monocytes Adriana R
    University of Connecticut OpenCommons@UConn UCHC Articles - Research University of Connecticut Health Center Research 1-2008 Phagocytosis of Borrelia burgdorferi, the Lyme Disease Spirochete, Potentiates Innate Immune Activation and Induces Apoptosis in Human Monocytes Adriana R. Cruz University of Connecticut School of Medicine and Dentistry Meagan W. Moore University of Connecticut School of Medicine and Dentistry Carson J. La Vake University of Connecticut School of Medicine and Dentistry Christian H. Eggers University of Connecticut School of Medicine and Dentistry Juan C. Salazar University of Connecticut School of Medicine and Dentistry See next page for additional authors Follow this and additional works at: https://opencommons.uconn.edu/uchcres_articles Part of the Medicine and Health Sciences Commons Recommended Citation Cruz, Adriana R.; Moore, Meagan W.; La Vake, Carson J.; Eggers, Christian H.; Salazar, Juan C.; and Radolf, Justin D., "Phagocytosis of Borrelia burgdorferi, the Lyme Disease Spirochete, Potentiates Innate Immune Activation and Induces Apoptosis in Human Monocytes" (2008). UCHC Articles - Research. 182. https://opencommons.uconn.edu/uchcres_articles/182 Authors Adriana R. Cruz, Meagan W. Moore, Carson J. La Vake, Christian H. Eggers, Juan C. Salazar, and Justin D. Radolf This article is available at OpenCommons@UConn: https://opencommons.uconn.edu/uchcres_articles/182 INFECTION AND IMMUNITY, Jan. 2008, p. 56–70 Vol. 76, No. 1 0019-9567/08/$08.00ϩ0 doi:10.1128/IAI.01039-07 Copyright © 2008, American Society for Microbiology. All Rights Reserved. Phagocytosis of Borrelia burgdorferi, the Lyme Disease Spirochete, Potentiates Innate Immune Activation and Induces Apoptosis in Human Monocytesᰔ Adriana R. Cruz,1†‡ Meagan W. Moore,1† Carson J.
    [Show full text]
  • Canine Lyme Borrelia
    Canine Lyme Borrelia Borrelia burgdorferi bacteria are the cause of Lyme disease in humans and animals. They can be visualized by darkfild microscopy as "corkscrew-shaped" motile spirochetes (400 x). Inset: The black-legged tick, lxodes scapularis (deer tick), may carry and transmit Borrelia burgdorferi to humans and animals during feeding, and thus transmit Lyme disease. Samples: Blood EDTA-blood as is, purple-top tubes or EDTA-blood preserved in sample buffer (preferred) Body fluids Preserved in sample buffer Notes: Send all samples at room temperature, preferably preserved in sample buffer MD Submission Form Interpretation of PCR Results: High Positive Borrelia spp. infection (interpretation must be correlated to (> 500 copies/ml swab) clinical symptoms) Low Positive (<500 copies/ml swab) Negative Borrelia spp. not detected Lyme Borreliosis Lyme disease is caused by spirochete bacteria of a subgroup of Borrelia species, called Borrelia burgdorferi sensu lato. Only one species, B. burgdorferi sensu stricto, is known to be present in the USA, while at least four pathogenic species, B. burgdorferi sensu stricto, B. afzelii, B. garinii, B. japonica have been isolated in Europe and Asia (Aguero- Rosenfeld et al., 2005). B. burgdorferi sensu lato organisms are corkscrew-shaped, motile, microaerophilic bacteria of the order Spirochaetales. Hard-shelled ticks of the genus Ixodes transmit B. burgdorferi by attaching and feeding on various mammalian, avian, and reptilian hosts. In the northeastern states of the US Ixodes scapularis, the black-legged deer tick, is the predominant vector, while at the west coast Lyme borreliosis is maintained by a transmission cycle which involves two tick species, I.
    [Show full text]
  • Borrelia Burgdorferi and Treponema Pallidum: a Comparison of Functional Genomics, Environmental Adaptations, and Pathogenic Mechanisms
    PERSPECTIVE SERIES Bacterial polymorphisms Martin J. Blaser and James M. Musser, Series Editors Borrelia burgdorferi and Treponema pallidum: a comparison of functional genomics, environmental adaptations, and pathogenic mechanisms Stephen F. Porcella and Tom G. Schwan Laboratory of Human Bacterial Pathogenesis, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, NIH, Hamilton, Montana, USA Address correspondence to: Tom G. Schwan, Rocky Mountain Laboratories, 903 South 4th Street, Hamilton, Montana 59840, USA. Phone: (406) 363-9250; Fax: (406) 363-9445; E-mail: [email protected]. Spirochetes are a diverse group of bacteria found in (6–8). Here, we compare the biology and genomes of soil, deep in marine sediments, commensal in the gut these two spirochetal pathogens with reference to their of termites and other arthropods, or obligate parasites different host associations and modes of transmission. of vertebrates. Two pathogenic spirochetes that are the focus of this perspective are Borrelia burgdorferi sensu Genomic structure lato, a causative agent of Lyme disease, and Treponema A striking difference between B. burgdorferi and T. pal- pallidum subspecies pallidum, the agent of venereal lidum is their total genomic structure. Although both syphilis. Although these organisms are bound togeth- pathogens have small genomes, compared with many er by ancient ancestry and similar morphology (Figure well known bacteria such as Escherichia coli and Mycobac- 1), as well as by the protean nature of the infections terium tuberculosis, the genomic structure of B. burgdorferi they cause, many differences exist in their life cycles, environmental adaptations, and impact on human health and behavior. The specific mechanisms con- tributing to multisystem disease and persistent, long- term infections caused by both organisms in spite of significant immune responses are not yet understood.
    [Show full text]
  • Investigation of the Lipoproteome of the Lyme Disease Bacterium
    INVESTIGATION OF THE LIPOPROTEOME OF THE LYME DISEASE BACTERIUM BORRELIA BURGDORFERI BY Alexander S. Dowdell Submitted to the graduate degree program in Microbiology, Molecular Genetics & Immunology and the Graduate Faculty of the University of Kansas in partial fulfillment of the requirements for the degree of Doctor of Philosophy. _____________________________ Wolfram R. Zückert, Ph.D., Chairperson _____________________________ Indranil Biswas, Ph.D. _____________________________ Mark Fisher, Ph.D. _____________________________ Joe Lutkenhaus, Ph.D. _____________________________ Michael Parmely, Ph.D. Date Defended: April 27th, 2017 The dissertation committee for Alexander S. Dowdell certifies that this is the approved version of the following dissertation: INVESTIGATION OF THE LIPOPROTEOME OF THE LYME DISEASE BACTERIUM BORRELIA BURGDORFERI _____________________________ Wolfram R. Zückert, Ph.D., Chairperson Date Approved: May 4th, 2017 ii Abstract The spirochete bacterium Borrelia burgdorferi is the causative agent of Lyme borreliosis, the top vector-borne disease in the United States. B. burgdorferi is transmitted by hard- bodied Ixodes ticks in an enzootic tick/vertebrate cycle, with human infection occurring in an accidental, “dead-end” fashion. Despite the estimated 300,000 cases that occur each year, no FDA-approved vaccine is available for the prevention of Lyme borreliosis in humans. Development of new prophylaxes is constrained by the limited understanding of the pathobiology of B. burgdorferi, as past investigations have focused intensely on just a handful of identified proteins that play key roles in the tick/vertebrate infection cycle. As such, identification of novel B. burgdorferi virulence factors is needed in order to expedite the discovery of new anti-Lyme therapeutics. The multitude of lipoproteins expressed by the spirochete fall into one such category of virulence factor that merits further study.
    [Show full text]
  • Assessing Lyme Disease Relevant Antibiotics Through Gut Bacteroides Panels
    Assessing Lyme Disease Relevant Antibiotics through Gut Bacteroides Panels by Sohum Sheth Abstract: Lyme borreliosis is the most prevalent vector-borne disease in the United States caused by the transmission of bacteria Borrelia burgdorferi harbored by the Ixodus scapularis ticks (Sharma, Brown, Matluck, Hu, & Lewis, 2015). Antibiotics currently used to treat Lyme disease include oral doxycycline, amoxicillin, and ce!riaxone. Although the current treatment is e"ective in most cases, there is need for the development of new antibiotics against Lyme disease, as the treatment does not work in 10-20% of the population for unknown reasons (X. Wu et al., 2018). Use of antibiotics in the treatment of various diseases such as Lyme disease is essential; however, the downside is the development of resistance and possibly deleterious e"ects on the human gut microbiota composition. Like other organs in the body, gut microbiota play an essential role in the health and disease state of the body (Ianiro, Tilg, & Gasbarrini, 2016). Of importance in the microbiome is the genus Bacteroides, which accounts for roughly one-third of gut microbiome composition (H. M. Wexler, 2007). $e purpose of this study is to investigate how antibiotics currently used for the treatment of Lyme disease in%uences the Bacteroides cultures in vitro and compare it with a new antibiotic (antibiotic X) identi&ed in the laboratory to be e"ective against B. burgdorferi. Using microdilution broth assay, minimum inhibitory concentration (MIC) was tested against nine di"erent strains of Bacteroides. Results showed that antibiotic X has a higher MIC against Bacteroides when compared to amoxicillin, ce!riaxone, and doxycycline, making it a promising new drug for further investigation and in vivo studies.
    [Show full text]
  • Treponema Borrelia Family: Leptospiraceae Genus: Leptospira Gr
    Bacteriology lecture no.12 Spirochetes 3rd class -The spirochetes: are a large ,heterogeneous group of spiral ,motile bacteria. Although, • there are at least eight genera in this family ,only the genera Treponema,Borrelia,and Leptospira which contain organism pathogenic for humans . -There are some reports of intestinal spirochetes ,that have been isolated from biopsy material ,these are Brachyspira pilosicoli,and Brachyspira aalborgi. *Objectives* Taxonomy Order: Spirochaetales Family: Spirochaetaceae Genus: Treponema Borrelia Family: Leptospiraceae Genus: Leptospira -Gram-negative spirochetes -Spirochete from Greek for “coiled hair "they are : *1*Extremely thin and can be very long *2* Motile by periplasmic flagella (axial fibrils or endoflagella) *3*Outer sheath encloses axial fibrils *4*Axial fibrils originate from insertion pores at both poles of cell 1 Bacteriology lecture no.12 Spirochetes 3rd class Spirochaetales Associated Human Diseases Treponema Main Treponema are: - T. pallidum subspecies pallidum - Syphilis: Venereal (sexual) disease 2 Bacteriology lecture no.12 Spirochetes 3rd class - T. pertenue - Yaws Non venereal - T. carateum - Pinta skin disease All three species are morphologically identical Characteristics of T.pallidum 1-They are long ,slender ,helically coiled ,spiral or cork –screw shaped bacilli. 2-T.pallidum has an outer sheath or glycosaminoglycan contain peptidoglycan and maintain the structural integrity of the organisms. 3-Endoflagella (axial filament ) are the flagella-like organelles in the periplasmic space encased by the outer membranes . 4-The endoflagella begin at each end of the organism and wind around it ,extending to and overlapping at the midpoint. 5- Inside the endoflagella is the inner membrane (cytoplasmic membrane)that provide osmotic stability and cover the protoplasmic cylinders .
    [Show full text]
  • Circulation of Pathogenic Spirochetes in the Genus Borrelia
    CIRCULATION OF PATHOGENIC SPIROCHETES IN THE GENUS BORRELIA WITHIN TICKS AND SEABIRDS IN BREEDING COLONIES OF NEWFOUNDLAND AND LABRADOR by © Hannah Jarvis Munro A Thesis submitted to the School of Graduate Studies in partial fulfillment of the requirements for the degree of Doctor of Philosophy Department of Biology Memorial University of Newfoundland May 2018 St. John’s, Newfoundland and Labrador ABSTRACT Birds are the reservoir hosts of Borrelia garinii, the primary causative agent of neurological Lyme disease. In 1991 it was also discovered in the seabird tick, Ixodes uriae, in a seabird colony in Sweden, and subsequently has been found in seabird ticks globally. In 2005, the bacterium was found in seabird colonies in Newfoundland and Labrador (NL); representing its first documentation in the western Atlantic and North America. In this thesis, aspects of enzootic B. garinii transmission cycles were studied at five seabird colonies in NL. First, seasonality of I. uriae ticks in seabird colonies observed from 2011 to 2015 was elucidated using qualitative model-based statistics. All instars were found throughout the June-August study period, although larvae had one peak in June, and adults had two peaks (in June and August). Tick numbers varied across sites, year, and with climate. Second, Borrelia transmission cycles were explored by polymerase chain reaction (PCR) to assess Borrelia spp. infection prevalence in the ticks and by serological methods to assess evidence of infection in seabirds. Of the ticks, 7.5% were PCR-positive for B. garinii, and 78.8% of seabirds were sero-positive, indicating that B. garinii transmission cycles are occurring in the colonies studied.
    [Show full text]
  • Borrelia Burgdorferi)
    The Lyme Bacterium (Borrelia burgdorferi) Habitat : Called an endoparasite, this bacterium can only live inside of another organism. Remarkably, B. burgforferi can survive in a range of temperatures, from the hemolymph of insects to the warm blood of mammals. Diet : B. burgforferi obtains nutrients and energy from the blood of a host. Life Cycle/Reproduction: B. burgforferi reproduces asexually, making identical copies of itself with each duplication. They can reproduce rapidly, and one scientific study found an average of 2,735 bacteria/tick 15 days after the tick had fed. Although the scientists found that recently molted nymphs had only 300 bacteria/nymph, within 75 days, these nymphs had an average of 61,275 bacteria! The tick serves as the vector for the bacteria, moving it from one “holding place” or “reservoir” to another host, which may even be a human. Small rodents, especially mice, act as good reservoirs. If a larva bites an infected mouse, that tick will likely become infected itself. The tick vector can then bite another host and transmit the bacteria, propagating itself. Dispersal: There are two types of dispersal associated with this bacterium. First, there is dispersal of individual bacteria. For example within the tick, the bacteria attach to the mid-gut to avoid being digested by the tick. When the tick attaches to a vertebrate host, the bacteria detach from the mid-gut and migrate to the salivary glands, where they can then be transmitted to the vertebrate host. Secondly, there is dispersal of the entire population of bacteria. This type of dispersal requires that the bacteria successfully “move” from a reservoir to a host with the help of a vector.
    [Show full text]
  • Microbial Communities Associated with the Camel Tick, Hyalomma Dromedarii
    www.nature.com/scientificreports OPEN Microbial communities associated with the camel tick, Hyalomma dromedarii: 16S rRNA gene‑based analysis Nighat Perveen, Sabir Bin Muzafar, Ranjit Vijayan & Mohammad Ali Al‑Deeb* Hyalomma dromedarii is an important blood‑feeding ectoparasite that afects the health of camels. We assessed the profle of bacterial communities associated with H. dromedarii collected from camels in the eastern part of the UAE in 2010 and 2019. A total of 100 partially engorged female ticks were taken from tick samples collected from camels (n = 100; 50/year) and subjected to DNA extraction and sequencing. The 16S rRNA gene was amplifed from genomic DNA and sequenced using Illumina MiSeq platform to elucidate the bacterial communities. Principle Coordinates Analysis (PCoA) was conducted to determine patterns of diversity in bacterial communities. In 2010 and 2019, we obtained 899,574 and 781,452 read counts and these formed 371 and 191 operational taxonomic units (OTUs, clustered at 97% similarity), respectively. In both years, twenty‑fve bacterial families with high relative abundance were detected and the following were the most common: Moraxellaceae, Enterobacteriaceae, Staphylococcaceae, Bacillaceae, Corynebacteriaceae, Flavobacteriaceae, Francisellaceae, Muribaculaceae, Neisseriaceae, and Pseudomonadaceae. Francisellaceae and Enterobacteriaceae coexist in H. dromedarii and we suggest that they thrive under similar conditions and microbial interactions inside the host. Comparisons of diversity indicated that microbial communities difered in terms of richness and evenness between 2010 and 2019, with higher richness but lower evenness in communities in 2010. Principle coordinates analyses showed clear clusters separating microbial communities in 2010 and 2019. The diferences in communities suggested that the repertoire of microbial communities have shifted.
    [Show full text]
  • Borrelia Burgdorferi Igg, Igm Fully Automated Chemiluminescence Assays for an Accurate Detection of Igg and Igm Antibodies to Borrelia Burgdorferi
    Infectious Disease Borrelia burgdorferi IgG, IgM Fully automated chemiluminescence assays for an accurate detection of IgG and IgM antibodies to Borrelia Burgdorferi FOR OUTSIDE THE US AND CANADA ONLY Infectious Disease Borrelia burgdorferi IgG, IgM Searching for diagnostic clarity: Unique selection of raw materials LIAISON® Borrelia serology line The diagnosis of Lyme borreliosis is based on clinical The LIAISON® Borrelia assays are based on recombinant proteins manifestations and history of exposure to ticks in an endemic that allow reduction of cross-reactivity problems providing area. Clinical manifestation of Lyme borreliosis may be similar higher specificity in comparison with whole-cell lysate assays. to that of other diseases, and serological detection of Borrelia The use of immunodominant Borrelia antigens, VIsE for IgG antibodies represents a fundamental aid to diagnosis (Fig.1). assay, OspC and VlsE for IgM assay, has improved the diagnostic sensitivity in all stages of Lyme infection. Tests with high diagnostic accuracy are particularly important for differential diagnosis since additional factors complicate • LIAISON® Borrelia IgG features the antigen VlsE, an serological findings: outer surface lipoprotein playing a major role in the immune response to Lyme disease and leading to decisive • early stage of infection may not show a measurable immune increase of sensitivity in neuroborreliosis (NB). The response VlsE antigen is poorly represented in whole-cell lysate obtained from in vitro cultured B. burgdorferi. • IgM antibodies may persist for months • LIAISON® Borrelia IgM II uses two recombinant antigens: • cross-reaction with other spirochaete proteins, or other OspC, an outer surface protein highly specific for infectious diseases or autoimmune disorders may cause IgM detection in the early phase of infection, and the false positive antibody response VlsE protein.
    [Show full text]
  • The Brilliance of Borrelia: Mechanisms of Host Immune Evasion by Lyme Disease-Causing Spirochetes
    pathogens Review The Brilliance of Borrelia: Mechanisms of Host Immune Evasion by Lyme Disease-Causing Spirochetes Cassidy Anderson and Catherine A. Brissette * Department of Biomedical Sciences, University of North Dakota, Grand Forks, ND 58202, USA; [email protected] * Correspondence: [email protected]; Tel.: +1-701-777-6412 Abstract: Lyme disease (LD) has become the most common vector-borne illness in the northern hemisphere. The causative agent, Borrelia burgdorferi sensu lato, is capable of establishing a persistent infection within the host. This is despite the activation of both the innate and adaptive immune responses. B. burgdorferi utilizes several immune evasion tactics ranging from the regulation of surface proteins, tick saliva, antimicrobial peptide resistance, and the disabling of the germinal center. This review aims to cover the various methods by which B. burgdorferi evades detection and destruction by the host immune response, examining both the innate and adaptive responses. By understanding the methods employed by B. burgdorferi to evade the host immune response, we gain a deeper knowledge of B. burgdorferi pathogenesis and Lyme disease, and gain insight into how to create novel, effective treatments. Keywords: Lyme disease; Borrelia; immune response; innate; adaptive; complement Citation: Anderson, C.; Brissette, C.A. The Brilliance of Borrelia: 1. Introduction Mechanisms of Host Immune Since the first investigations conducted by Steere and Malawista in 1975 [1,2], Lyme Evasion by Lyme Disease-Causing borreliosis, otherwise known as Lyme disease (LD), has become the most common vector- Spirochetes. Pathogens 2021, 10, 281. borne illness in the northern hemisphere [3]. LD is caused by infection with a member of https://doi.org/10.3390/pathogens the Borrelia burgdorferi sensu lato (s.l.) complex.
    [Show full text]