Borrelia burgdorferi: Difference between revisions
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{{Taxobox | {{Taxobox | ||
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==Description and Significance== | ==Description and Significance== | ||
''Borrelia burgdorferi'' are | ''Borrelia burgdorferi'' are Gram-negative spirochetes found primarily in North America and Europe. It is a double membraned, motile, spiral shaped microorganism that inhabits the gut of deer ticks (''Ixodes scapularis'').<ref name=description>{{Cite journal | ||
| doi = 10.1099/00207713-34-4-496 | | doi = 10.1099/00207713-34-4-496 | ||
| volume = 34 | | volume = 34 | ||
Line 86: | Line 85: | ||
}}</ref> It contains serum-supplemented mammalian tissue-culture that enables the bacterium to reproduce without ever having the need to synthesize too many biological compounds. | }}</ref> It contains serum-supplemented mammalian tissue-culture that enables the bacterium to reproduce without ever having the need to synthesize too many biological compounds. | ||
The sequencing showed 853 open reading frames, with an average size of 992 base pairs. 93% of the genome represents coding sequence, and 59% were assigned biological roles. Most of the chromosomal genes code for a basic set of proteins that are required for DNA replication, transcription, translation, solute transport and energy metabolism.<ref name=genetics | The sequencing showed 853 open reading frames, with an average size of 992 base pairs. 93% of the genome represents coding sequence, and 59% were assigned biological roles. Most of the chromosomal genes code for a basic set of proteins that are required for DNA replication, transcription, translation, solute transport and energy metabolism.<ref name=genetics /><ref>{{Cite journal | ||
| issn = 0950-382X | | issn = 0950-382X | ||
| volume = 35 | | volume = 35 | ||
Line 113: | Line 98: | ||
| year = 2000 | | year = 2000 | ||
| url = http://www.ncbi.nlm.nih.gov/pubmed/10672174 | | url = http://www.ncbi.nlm.nih.gov/pubmed/10672174 | ||
}}</ref><ref name=map>{{Cite journal | |||
| doi = 10.1093/nar/gki075 | |||
| volume = 33 | |||
| issue = suppl_1 | |||
| pages = D317-320 | |||
| last = Stothard | |||
| first = Paul | |||
| coauthors = Gary Van Domselaar, Savita Shrivastava, Anchi Guo, Brian O'Neill, Joseph Cruz, Michael Ellison, David S. Wishart | |||
| title = BacMap: an interactive picture atlas of annotated bacterial genomes | |||
| journal = Nucl. Acids Res. | |||
| accessdate = 2009-05-11 | |||
| date = 2005-01-01 | |||
| url = http://nar.oxfordjournals.org/cgi/content/abstract/33/suppl_1/D317 | |||
}}</ref> | }}</ref> | ||
{{Image|Borrelia genome.png|right|400px|This image shows a recent mapping of B. burgdorferi genome. Click to enlarge.}} | |||
{| class="wikitable" | {| class="wikitable" | ||
|+DNA Molecule Summary | |+DNA Molecule Summary | ||
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==Cell Structure== | ==Cell Structure== | ||
''B. burgdorferi'' are long | ''B. burgdorferi'' are long Gram-negative spirochetes, although some researchers however claim that the organism does not exhibit properties of either Gram-positive or Gram-negative bacteria since they do not exhibit defining Gram-negative characteristics. Stained cells are visible by dark-field or phase-contrast microscopy, but not visible by bright field microscopy. They are flexible helical cells and are much longer than they are wide. They usually have a length of 20-30 μm but a width of only 0.2-0.3 μm. The organism is motile with both rotational and translational movements, and the coiling of cells is regular. On the average, seven periplasmic flagella are located at each cell end, and these flagella overlap at the central region of the cell. There are multiple layers of membrane that surround the protoplasmic layer, cytoplasmic membrane, and the enclosed cytoplasmic contents.<ref name= description/> | ||
==Metabolism== | ==Metabolism== | ||
''B. Burgdorferi'' are classified as being chemoorganotropic, and derive energy by metabolizing organic molecules. The organism is microaerophilic; they require oxygen to survive, but only at low concentrations. Too much or lack of oxygen can be harmful to them. They cannot synthesize their own amino acids, fatty acids, enzyme cofactors, and nucleotides. They also happen to be catalase negative; they are unable to break down hydrogen peroxide. It is possible to cultivate the organism in vitro, but it requires a very complex growth medium since it lacks the ability to synthesize various necessary compound (see genome structure). The medium used to grow ''Borrelia burgdorferi'' is called Barbour-Stoenner-Kelly (BSK) medium. It contains over thirteen ingredients in a rabbit serum base. | ''B. Burgdorferi'' are classified as being chemoorganotropic, and derive energy by metabolizing organic molecules.<ref name=description/> The organism is microaerophilic; they require oxygen to survive, but only at low concentrations. Too much or lack of oxygen can be harmful to them. They cannot synthesize their own amino acids, fatty acids, enzyme cofactors, and nucleotides. They also happen to be catalase negative; they are unable to break down hydrogen peroxide. It is possible to cultivate the organism in vitro, but it requires a very complex growth medium since it lacks the ability to synthesize various necessary compound (see genome structure). The medium used to grow ''Borrelia burgdorferi'' is called Barbour-Stoenner-Kelly (BSK) medium. It contains over thirteen ingredients in a rabbit serum base.<ref name=bsk>{{Cite journal | ||
| volume = 25 | |||
| issue = 11 | |||
| pages = 2054-2058 | |||
| last = Kurtti | |||
| first = T J | |||
| coauthors = U G Munderloh, R C Johnson, G G Ahlstrand | |||
| title = Colony formation and morphology in Borrelia burgdorferi. | |||
| journal = J. Clin. Microbiol. | |||
| accessdate = 2009-05-11 | |||
| date = 1987-11-01 | |||
| url = http://jcm.asm.org/cgi/content/abstract/25/11/2054 | |||
}}</ref> | |||
==Ecology== | ==Ecology== | ||
The optimal growth temperature is 34° to 37°C, and the organism has a generation time of 11 to 12 hours at 35°C.<ref name=description/> Their life cycle is directly linked to their host, and they depend on arthropod vectors (ticks) to infect mammals. They reside in infected mammals as well as in the gut of ticks.<ref name=book/> They multiply when there is enough blood ingested by the tick to support bacterial growth. | |||
The optimal growth temperature is 34° to 37°C, and the organism has a generation time of 11 to 12 hours at 35°C. Their life cycle is directly linked to their host, and they depend on arthropod vectors (ticks) to infect mammals. They reside in infected mammals as well as in the gut of ticks. They multiply when there is enough blood ingested by the tick to support bacterial growth. | {{Image|Deer Tick lifecycle.jpg|center|400px|Tick Life Cycle. Click Image To Enlarge}} | ||
The vector tick, ''Ixodes scapularis'', undergoes a two year life cycle beginning when the female drops from her animal host to lay eggs in the soil during the spring. Very small larvae emerge during the summer and attach to a passing small animal (such as mouse) to feed on its blood. If the small animal is infected with the spirochete, the larve become infected as they feed. Fed larvae drop back to the ground and molt into nymphs. Nymphs wait until next year's warm weather to search for another host to feed on before becoming adult ticks. They prefer the white-footed mouse, but will take any warm-blooded host that happens along. At this point, the infected nymphs can infect new animal hosts (including human). The fed nymph falls back to earth to molt, and emerge as an adult tick. The adult has one more blood feeding before it mates by late spring, and infected nymphs carry the infection into adulthood. Male ticks die following mating, while female ticks die after laying eggs, thus, completing the life cycle. <ref name=barnes>{{Cite book | last=Barnes | first=Ethne | authorlink=Ethne Barnes | coauthors= | title=Diseases and human evolution | date=2005 | publisher=University of New Mexico Press | location=Albuquerque | isbn=0826330657 | pages=376-379}}</ref> | |||
The vector tick, ''Ixodes scapularis'', undergoes a two year life cycle beginning when the female drops from her animal host to lay eggs in the soil during the spring. Very small larvae emerge during the summer and attach to a passing small animal (such as mouse) to feed on its blood. If the small animal is infected with the spirochete, the larve become infected as they feed. Fed larvae drop back to the ground and molt into nymphs. Nymphs wait until next year's warm weather to search for another host to feed on before becoming adult ticks. They prefer the white-footed mouse, but will take any warm-blooded host that happens along. At this point, the infected nymphs can infect new animal hosts (including human). The fed nymph falls back to earth to molt, and emerge as an adult tick. The adult has one more blood feeding before it mates by late spring, and infected nymphs carry the infection into adulthood. Male ticks die following mating, while female ticks die after laying eggs, thus, completing the life cycle | |||
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}}</ref | |||
==Pathology== | ==Pathology== | ||
{{Image|Adult Tick.jpg|right|150px| ''Ixodes scapularis'', or Deer Tick.}} | |||
{{Image|Deer tick all.jpg|right|350px|This image shows the relative sizes of male, female, nymph, and larval ticks (''Ixodes scapularis''). Nymphs are the best candidates for transmission, since they are relatively small and much harder to detect.}} | {{Image|Deer tick all.jpg|right|350px|This image shows the relative sizes of male, female, nymph, and larval ticks (''Ixodes scapularis''). Nymphs are the best candidates for transmission, since they are relatively small and much harder to detect.}} | ||
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}}</ref> | }}</ref> | ||
Most incidences of Lyme disease occur from May through September because the nymphal stage of the tick is responsible for most cases. They are too small to be easily detectable, and their bites cause much milder pain than an adult tick.<ref name=emedicine/> The symptoms are divided into three stages, each stage being more advanced than the previous. Initial sign and sympotoms of Lyme disease include an appearance of a rash, which has the appearance of being solid red or bull’s eye rash with flu like symptoms.<ref name=emedicine>http://emedicine.medscape.com/article/1053863-overview</ref> These symptoms may appear up to a month after infection. Within weeks of these initial | Most incidences of Lyme disease occur from May through September because the nymphal stage of the tick is responsible for most cases. They are too small to be easily detectable, and their bites cause much milder pain than an adult tick.<ref name=emedicine/> The symptoms are divided into three stages, each stage being more advanced than the previous. Initial sign and sympotoms of Lyme disease include an appearance of a rash, which has the appearance of being solid red or bull’s eye rash with flu like symptoms.<ref name=emedicine>http://emedicine.medscape.com/article/1053863-overview</ref> These symptoms may appear up to a month after infection. Within weeks of these initial stage one symptoms however, the bacterium may spread to various other parts of the body through the bloodstream. At this point, the disease can progress to stage two, and infected individuals may start having acute neurological problems such as Bell's Palsy. 15% of untreated patients progress to this stage. <ref name=stats>{{Cite journal | ||
| doi = 10.1017/S1462399404007276 | | doi = 10.1017/S1462399404007276 | ||
| volume = 6 | | volume = 6 | ||
Line 202: | Line 198: | ||
| date = 2004 | | date = 2004 | ||
| url = http://journals.cambridge.org/action/displayAbstract?fromPage=online&aid=202506 | | url = http://journals.cambridge.org/action/displayAbstract?fromPage=online&aid=202506 | ||
}}</ref> Meningitis as well as mild Encephalitis is also common at this stage, leading to memory loss, sleep disturbances, or changes in mood or affect. The third | }}</ref> Meningitis as well as mild Encephalitis is also common at this stage, leading to memory loss, sleep disturbances, or changes in mood or affect. The third and the most severe stage may occur months to years after initial infection.<ref name=emedicine/> Symptoms at this stage are primarily rheumatologic and neurologic, and mostly untreatable. | ||
'''Stage 1 – Early localized infection''' | |||
*Skin Rash Around Tick Bite (75%) | |||
*Mild Illness | |||
*Flu-like Symptoms | |||
*Fevers | |||
*Chills | |||
*Swollen Lymph Nodes | |||
*Headache | |||
*Stiff Neck | |||
*Muscle Fatigue | |||
'''Stage 2 – Early Disseminated Infection''' | |||
*Neurological Problems | |||
*Meningitis | |||
*Encephalitis | |||
'''Stage 3 – Late Persistent Infection''' | |||
*Polyneuropathy | |||
*Pain and Numbness | |||
*Cognitive Impairment | |||
*Arthritis | |||
*Acrodermatitis chronica atrophicans (primarily in Europe) | |||
==Current Research== | ==Current Research== | ||
Researchers are currently attempting to uncover what exactly it is that makes the bacterium pathogenic to humans. Much of the research is directed to the genetics and certain proteins of ''B. burgdorferi'' that seem to contribute to its pathogenesis. | |||
One of the proposed idea involves a subset of the genetically distinct lineages found in every ''B. burgdorferi'' population where the newly transmitted parasites are selected for best utilizing its new ecological niche. This idea is still debated, as it implies the possibility of multiple mechanism of infection. <ref name=sbu>{{Cite journal | |||
| volume = 78 | |||
| issue = 5 | |||
| pages = 806-810 | |||
| last = Dykhuizen | |||
| first = Daniel E. | |||
| coauthors = Dustin Brisson, Sabina Sandigursky, Gary P. Wormser, John Nowakowski, Robert B. Nadelman, Ira Schwartz | |||
| title = The Propensity of Different Borrelia burgdorferi sensu stricto Genotypes to Cause Disseminated Infections in Humans | |||
| journal = Am J Trop Med Hyg | |||
| accessdate = 2009-05-11 | |||
| date = 2008-05-01 | |||
| url = http://www.ajtmh.org/cgi/content/abstract/78/5/806 | |||
}}</ref> In a paper titled "The Propensity of Different Borrelia burgdorferi sensu stricto Genotypes to Cause Disseminated Infections in Humans,"<ref name=sbu/> researchers challenged the idea that only certain genotypes of B. burgdorferi cause pathogenesis in humans or other mammals. Their results indicate that all genotypes of the bacterium have the potential to become pathogenic in humans, but some are much more likely than others to do so. | |||
In 2008, researches discovered that the saliva of deer ticks (''Ixodes ricinus'') seem to effect the proliferation of B. burgdorferi in mammals.<ref name=saliva>{{Cite journal | |||
| doi = 10.1016/j.ijmm.2008.10.009 | |||
| issn = 1438-4221 | |||
| volume = In Press, Corrected Proof | |||
| last = Horká | |||
| first = Helena | |||
| coauthors = Katerina Cerná-Kýcková, Anna Skallová, Jan Kopecký | |||
| title = Tick saliva affects both proliferation and distribution of Borrelia burgdorferi spirochetes in mouse organs and increases transmission of spirochetes to ticks | |||
| journal = International Journal of Medical Microbiology | |||
| accessdate = 2009-05-11 | |||
| url = http://www.sciencedirect.com/science/article/B7GW0-4VCNF4P-1/2/ca2368217c86033b36d5d6f5b44b1ae5 | |||
}}</ref> Mice were injected with the bacterium while being fed on by uninfected ticks, and the proliferation of the bacterium was compared to mice that were injected with the bacterium while not being fed on by ticks. The results show a very early effect of tick saliva on the proliferation and distribution of Borrelia spirochetes in the host, probably due to the effect of saliva on the host innate immunity mechanisms.<ref name=saliva/> | |||
A paper published in January 2009 investigated earlier claims of Lyme disease vaccination being linked to destructive arthritis <ref name=art1>{{Cite journal | |||
| doi = 10.1128/CDLI.10.1.44-52.2003 | |||
| volume = 10 | |||
| issue = 1 | |||
| pages = 44-52 | |||
| last = Christopherson | |||
| first = John A. | |||
| coauthors = Erik L. Munson, Douglas M. England, Cindy L. Croke, Monica C. Remington, Melanie L. Molitor, David J. DeCoster, Steven M. Callister, Ronald F. Schell | |||
| title = Destructive Arthritis in Vaccinated Interferon Gamma-Deficient Mice Challenged with Borrelia burgdorferi: Modulation by Tumor Necrosis Factor Alpha | |||
| journal = Clin. Diagn. Lab. Immunol. | |||
| accessdate = 2009-05-11 | |||
| date = 2003-01-01 | |||
| url = http://cvi.asm.org/cgi/content/abstract/10/1/44 | |||
}}</ref><ref name=art2>{{Cite journal | |||
| volume = 62 | |||
| issue = 7 | |||
| pages = 2825-2833 | |||
| last = Lim | |||
| first = L C | |||
| coauthors = D M England, B K DuChateau, N J Glowacki, J R Creson, S D Lovrich, S M Callister, D A Jobe, R F Schell | |||
| title = Development of destructive arthritis in vaccinated hamsters challenged with Borrelia burgdorferi. | |||
| journal = Infect. Immun. | |||
| accessdate = 2009-05-11 | |||
| date = 1994-07-01 | |||
| url = http://iai.asm.org/cgi/content/abstract/62/7/2825 | |||
}}</ref>. Researchers compared cases of destructive arthritis in patients who received Lyme disease vaccine with three control groups; 1) inflammatory arthritis but not Lyme disease vaccine (arthritis controls), 2) Lyme disease vaccine but not inflammatory arthritis (vaccine controls), and 3) neither Lyme disease vaccine nor inflammatory arthritis (normal controls). HLA-DRB1 allele typing, Western blotting for Lyme antigen, and T cell reactivity testing were performed. Their results showed that Lyme disease vaccine is not a major factor in the development of arthritis.<ref name=art3>{{Cite journal | |||
| doi = 10.1002/art.24418 | |||
| volume = 60 | |||
| issue = 4 | |||
| pages = 1179-1186 | |||
| last = Ball | |||
| first = Robert | |||
| coauthors = Sean V. Shadomy, Abbie Meyer, Brigitte T. Huber, Mary S. Leffell, Andrea Zachary, Michael Belotto, Eileen Hilton, Marthe Bryant-Genevier, Martin E. Schriefer, Frederick W. Miller, M. Miles Braun | |||
| title = HLA type and immune response to <I>Borrelia burgdorferi</I> outer surface protein a in people in whom arthritis developed after Lyme disease vaccination | |||
| journal = Arthritis & Rheumatism | |||
| accessdate = 2009-05-11 | |||
| date = 2009 | |||
| url = http://dx.doi.org/10.1002/art.24418 | |||
}}</ref> | |||
==References== | ==References== | ||
<div class="references-small"><references/></div> | <div class="references-small"><references/></div>[[Category:Suggestion Bot Tag]] |
Latest revision as of 14:01, 22 July 2024
Borrelia burgdorferi | ||||||||||||||
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Scientific classification | ||||||||||||||
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Binomial name | ||||||||||||||
Borrelia burgdorferi |
Description and Significance
Borrelia burgdorferi are Gram-negative spirochetes found primarily in North America and Europe. It is a double membraned, motile, spiral shaped microorganism that inhabits the gut of deer ticks (Ixodes scapularis).[1] It is named after American scientist Willy Burgdorfer who in 1982 isolated and determined the bacterium to be the causative agent of Lyme disease.[2] Lyme disease is the most common tick-borne disease in the US.[3][1]
Genome structure
B. Burgdorferi is one of the first organisms to have its genome sequenced; it followed Haemophilus influenzae and Mycoplasma genitalium in 1995. [4] It was found to have a very small, but complex genome that contains linear chromosomal DNA and up to as many as 20 plasmids. A study in 1997 found the linear DNA to be composed of 910,725 base pairs with a G+C content of 28.6%. In addition to that, the plasmids contributed 533,000 more base pairs to the organism's genome. [5]
The organism's small genome lacks the genes that are necessary for the synthesis of amino acids, fatty acids, enzyme cofactors, and nucleotides. [5] In order for them to be cultured, a very special type of medium called Barbour-Stoenner-Kelly (BSK) medium is used. [6] It contains serum-supplemented mammalian tissue-culture that enables the bacterium to reproduce without ever having the need to synthesize too many biological compounds.
The sequencing showed 853 open reading frames, with an average size of 992 base pairs. 93% of the genome represents coding sequence, and 59% were assigned biological roles. Most of the chromosomal genes code for a basic set of proteins that are required for DNA replication, transcription, translation, solute transport and energy metabolism.[5][7][8]
Number | Percent | |
---|---|---|
Total Number of all DNA molecules: | 18 | 100.00% |
Total Size of all DNA molecules: | 1443725bp | 100.00% |
Total number of linear DNA bases: | 910,725bp | 63.1% |
Number of chromosomal G+C bases: | 256551bp | 28.5% |
Number | Percent | |
---|---|---|
Total genes: | 853 | 100.00% |
Protein coding genes: | 793 | 93% |
Genes assigned a role category: | 502 | 59% |
Genes not assigned a role category: | 51 | 6.26% |
Hypothetical genes: | 102 | 12% |
Cell Structure
B. burgdorferi are long Gram-negative spirochetes, although some researchers however claim that the organism does not exhibit properties of either Gram-positive or Gram-negative bacteria since they do not exhibit defining Gram-negative characteristics. Stained cells are visible by dark-field or phase-contrast microscopy, but not visible by bright field microscopy. They are flexible helical cells and are much longer than they are wide. They usually have a length of 20-30 μm but a width of only 0.2-0.3 μm. The organism is motile with both rotational and translational movements, and the coiling of cells is regular. On the average, seven periplasmic flagella are located at each cell end, and these flagella overlap at the central region of the cell. There are multiple layers of membrane that surround the protoplasmic layer, cytoplasmic membrane, and the enclosed cytoplasmic contents.[1]
Metabolism
B. Burgdorferi are classified as being chemoorganotropic, and derive energy by metabolizing organic molecules.[1] The organism is microaerophilic; they require oxygen to survive, but only at low concentrations. Too much or lack of oxygen can be harmful to them. They cannot synthesize their own amino acids, fatty acids, enzyme cofactors, and nucleotides. They also happen to be catalase negative; they are unable to break down hydrogen peroxide. It is possible to cultivate the organism in vitro, but it requires a very complex growth medium since it lacks the ability to synthesize various necessary compound (see genome structure). The medium used to grow Borrelia burgdorferi is called Barbour-Stoenner-Kelly (BSK) medium. It contains over thirteen ingredients in a rabbit serum base.[9]
Ecology
The optimal growth temperature is 34° to 37°C, and the organism has a generation time of 11 to 12 hours at 35°C.[1] Their life cycle is directly linked to their host, and they depend on arthropod vectors (ticks) to infect mammals. They reside in infected mammals as well as in the gut of ticks.[3] They multiply when there is enough blood ingested by the tick to support bacterial growth.
The vector tick, Ixodes scapularis, undergoes a two year life cycle beginning when the female drops from her animal host to lay eggs in the soil during the spring. Very small larvae emerge during the summer and attach to a passing small animal (such as mouse) to feed on its blood. If the small animal is infected with the spirochete, the larve become infected as they feed. Fed larvae drop back to the ground and molt into nymphs. Nymphs wait until next year's warm weather to search for another host to feed on before becoming adult ticks. They prefer the white-footed mouse, but will take any warm-blooded host that happens along. At this point, the infected nymphs can infect new animal hosts (including human). The fed nymph falls back to earth to molt, and emerge as an adult tick. The adult has one more blood feeding before it mates by late spring, and infected nymphs carry the infection into adulthood. Male ticks die following mating, while female ticks die after laying eggs, thus, completing the life cycle. [10]
Pathology
Borrelia Burgdorferi causes Lyme disease, and is transmitted to humans and other mammals by deer ticks(Ixodes scapularis). Lyme is a multisystem inflammatory disease that affects the skin in the early stage and then spreads to the joints, nervous system and may eventually affect the organ systems. The bite of an infected nymph or adult tick can only transmit Lyme disease after it attaches to the host for thirty six to forty eight hours. This is due to the initial lag time, and the generation time of B. Burgdorferi, which happens to be 12 hours (see ecology). Spirochetes waiting in the mid-gut of the tick only begin to multiply as the tick starts its blood meal. Then they migrate to the salivary glands where they are discharged into the host with the tick's saliva. It takes several hours before a large enough infectious dose of spirochetes can penetrate the new host. [11]
Most incidences of Lyme disease occur from May through September because the nymphal stage of the tick is responsible for most cases. They are too small to be easily detectable, and their bites cause much milder pain than an adult tick.[12] The symptoms are divided into three stages, each stage being more advanced than the previous. Initial sign and sympotoms of Lyme disease include an appearance of a rash, which has the appearance of being solid red or bull’s eye rash with flu like symptoms.[12] These symptoms may appear up to a month after infection. Within weeks of these initial stage one symptoms however, the bacterium may spread to various other parts of the body through the bloodstream. At this point, the disease can progress to stage two, and infected individuals may start having acute neurological problems such as Bell's Palsy. 15% of untreated patients progress to this stage. [13] Meningitis as well as mild Encephalitis is also common at this stage, leading to memory loss, sleep disturbances, or changes in mood or affect. The third and the most severe stage may occur months to years after initial infection.[12] Symptoms at this stage are primarily rheumatologic and neurologic, and mostly untreatable.
Stage 1 – Early localized infection
- Skin Rash Around Tick Bite (75%)
- Mild Illness
- Flu-like Symptoms
- Fevers
- Chills
- Swollen Lymph Nodes
- Headache
- Stiff Neck
- Muscle Fatigue
Stage 2 – Early Disseminated Infection
- Neurological Problems
- Meningitis
- Encephalitis
Stage 3 – Late Persistent Infection
- Polyneuropathy
- Pain and Numbness
- Cognitive Impairment
- Arthritis
- Acrodermatitis chronica atrophicans (primarily in Europe)
Current Research
Researchers are currently attempting to uncover what exactly it is that makes the bacterium pathogenic to humans. Much of the research is directed to the genetics and certain proteins of B. burgdorferi that seem to contribute to its pathogenesis.
One of the proposed idea involves a subset of the genetically distinct lineages found in every B. burgdorferi population where the newly transmitted parasites are selected for best utilizing its new ecological niche. This idea is still debated, as it implies the possibility of multiple mechanism of infection. [14] In a paper titled "The Propensity of Different Borrelia burgdorferi sensu stricto Genotypes to Cause Disseminated Infections in Humans,"[14] researchers challenged the idea that only certain genotypes of B. burgdorferi cause pathogenesis in humans or other mammals. Their results indicate that all genotypes of the bacterium have the potential to become pathogenic in humans, but some are much more likely than others to do so.
In 2008, researches discovered that the saliva of deer ticks (Ixodes ricinus) seem to effect the proliferation of B. burgdorferi in mammals.[15] Mice were injected with the bacterium while being fed on by uninfected ticks, and the proliferation of the bacterium was compared to mice that were injected with the bacterium while not being fed on by ticks. The results show a very early effect of tick saliva on the proliferation and distribution of Borrelia spirochetes in the host, probably due to the effect of saliva on the host innate immunity mechanisms.[15]
A paper published in January 2009 investigated earlier claims of Lyme disease vaccination being linked to destructive arthritis [16][17]. Researchers compared cases of destructive arthritis in patients who received Lyme disease vaccine with three control groups; 1) inflammatory arthritis but not Lyme disease vaccine (arthritis controls), 2) Lyme disease vaccine but not inflammatory arthritis (vaccine controls), and 3) neither Lyme disease vaccine nor inflammatory arthritis (normal controls). HLA-DRB1 allele typing, Western blotting for Lyme antigen, and T cell reactivity testing were performed. Their results showed that Lyme disease vaccine is not a major factor in the development of arthritis.[18]
References
- ↑ 1.0 1.1 1.2 1.3 1.4 Johnson, Russell C.; George P. Schmid, Fred W. Hyde, A. G. Steigerwalt, Don J. Brenner (1984). "Borrelia burgdorferi sp. nov.: Etiologic Agent of Lyme Disease". Int J Syst Bacteriol 34 (4): 496-497. DOI:10.1099/00207713-34-4-496. Retrieved on 2009-04-29. Research Blogging.
- ↑ Burgdorfer, W; AG Barbour, SF Hayes, JL Benach, E Grunwaldt, JP Davis (1982). "Lyme disease-a tick-borne spirochetosis?". Science 216 (4552): 1317-1319. DOI:10.1126/science.7043737. Retrieved on 2009-04-29. Research Blogging.
- ↑ 3.0 3.1 MD, Alan G. Barbour (1996-04-01). Lyme Disease: The Cause, the Cure, the Controversy, 1. The Johns Hopkins University Press. ISBN 0801852455.
- ↑ http://bioinfo.mbb.yale.edu/course/projects/final-4/
- ↑ 5.0 5.1 5.2 Fraser, Claire M.; Sherwood Casjens, Wai Mun Huang, Granger G. Sutton, Rebecca Clayton, Raju Lathigra, Owen White, Karen A. Ketchum, Robert Dodson, Erin K. Hickey, Michelle Gwinn, Brian Dougherty, Jean-Francois Tomb, Robert D. Fleischmann, Delwood Richardson, Jeremy Peterson, Anthony R. Kerlavage, John Quackenbush, Steven Salzberg, Mark Hanson, Rene van Vugt, Nanette Palmer, Mark D. Adams, Jeannine Gocayne, Janice Weidman, Teresa Utterback, Larry Watthey, Lisa McDonald, Patricia Artiach, Cheryl Bowman, Stacey Garland, Claire Fujii, Matthew D. Cotton, Kurt Horst, Kevin Roberts, Bonnie Hatch, Hamilton O. Smith, J. Craig Venter (1997-12-11). "Genomic sequence of a Lyme disease spirochaete, Borrelia burgdorferi". Nature 390 (6660): 580-586. DOI:10.1038/37551. ISSN 0028-0836. Retrieved on 2009-04-29. Research Blogging.
- ↑ Callister, S M; K L Case, W A Agger, R F Schell, R C Johnson, J L Ellingson (1990-02-01). "Effects of bovine serum albumin on the ability of Barbour-Stoenner-Kelly medium to detect Borrelia burgdorferi.". J. Clin. Microbiol. 28 (2): 363-365. Retrieved on 2009-04-29.
- ↑ Casjens, S; N Palmer, R van Vugt, W M Huang, B Stevenson, P Rosa, R Lathigra, G Sutton, J Peterson, R J Dodson, D Haft, E Hickey, M Gwinn, O White, C M Fraser (2000). "A bacterial genome in flux: the twelve linear and nine circular extrachromosomal DNAs in an infectious isolate of the Lyme disease spirochete Borrelia burgdorferi". Molecular Microbiology 35 (3): 490-516. ISSN 0950-382X. Retrieved on 2009-04-27.
- ↑ Stothard, Paul; Gary Van Domselaar, Savita Shrivastava, Anchi Guo, Brian O'Neill, Joseph Cruz, Michael Ellison, David S. Wishart (2005-01-01). "BacMap: an interactive picture atlas of annotated bacterial genomes". Nucl. Acids Res. 33 (suppl_1): D317-320. DOI:10.1093/nar/gki075. Retrieved on 2009-05-11. Research Blogging.
- ↑ Kurtti, T J; U G Munderloh, R C Johnson, G G Ahlstrand (1987-11-01). "Colony formation and morphology in Borrelia burgdorferi.". J. Clin. Microbiol. 25 (11): 2054-2058. Retrieved on 2009-05-11.
- ↑ Barnes, Ethne (2005). Diseases and human evolution. Albuquerque: University of New Mexico Press, 376-379. ISBN 0826330657.
- ↑ MD, Alan G. Barbour (1996-04-01). Lyme Disease: The Cause, the Cure, the Controversy, 1. The Johns Hopkins University Press. ISBN 0801852455.
- ↑ 12.0 12.1 12.2 http://emedicine.medscape.com/article/1053863-overview
- ↑ Auwaerter, Paul G.; John Aucott, J. Stephen Dumler (2004). "Lyme Borreliosis (Lyme Disease): Molecular and Cellular Pathobiology and Prospects for Prevention, Diagnosis and Treatment". Expert Reviews in Molecular Medicine 6 (02): 1-22. DOI:10.1017/S1462399404007276. Retrieved on 2009-05-06. Research Blogging.
- ↑ 14.0 14.1 Dykhuizen, Daniel E.; Dustin Brisson, Sabina Sandigursky, Gary P. Wormser, John Nowakowski, Robert B. Nadelman, Ira Schwartz (2008-05-01). "The Propensity of Different Borrelia burgdorferi sensu stricto Genotypes to Cause Disseminated Infections in Humans". Am J Trop Med Hyg 78 (5): 806-810. Retrieved on 2009-05-11.
- ↑ 15.0 15.1 Horká, Helena; Katerina Cerná-Kýcková, Anna Skallová, Jan Kopecký. "Tick saliva affects both proliferation and distribution of Borrelia burgdorferi spirochetes in mouse organs and increases transmission of spirochetes to ticks". International Journal of Medical Microbiology In Press, Corrected Proof. DOI:10.1016/j.ijmm.2008.10.009. ISSN 1438-4221. Retrieved on 2009-05-11. Research Blogging.
- ↑ Christopherson, John A.; Erik L. Munson, Douglas M. England, Cindy L. Croke, Monica C. Remington, Melanie L. Molitor, David J. DeCoster, Steven M. Callister, Ronald F. Schell (2003-01-01). "Destructive Arthritis in Vaccinated Interferon Gamma-Deficient Mice Challenged with Borrelia burgdorferi: Modulation by Tumor Necrosis Factor Alpha". Clin. Diagn. Lab. Immunol. 10 (1): 44-52. DOI:10.1128/CDLI.10.1.44-52.2003. Retrieved on 2009-05-11. Research Blogging.
- ↑ Lim, L C; D M England, B K DuChateau, N J Glowacki, J R Creson, S D Lovrich, S M Callister, D A Jobe, R F Schell (1994-07-01). "Development of destructive arthritis in vaccinated hamsters challenged with Borrelia burgdorferi.". Infect. Immun. 62 (7): 2825-2833. Retrieved on 2009-05-11.
- ↑ Ball, Robert; Sean V. Shadomy, Abbie Meyer, Brigitte T. Huber, Mary S. Leffell, Andrea Zachary, Michael Belotto, Eileen Hilton, Marthe Bryant-Genevier, Martin E. Schriefer, Frederick W. Miller, M. Miles Braun (2009). "HLA type and immune response to Borrelia burgdorferi outer surface protein a in people in whom arthritis developed after Lyme disease vaccination". Arthritis & Rheumatism 60 (4): 1179-1186. DOI:10.1002/art.24418. Retrieved on 2009-05-11. Research Blogging.