Lyme disease or Lyme borreliosis is the most common vector-borne disease in the Northern Hemisphere. Named after the town of Lyme, Connecticut, it is now one of the fastest growing infectious diseases in the U.S. Lyme disease is caused by infection with the spirochetal bacteria Borrelia burgdorferi, and is primarily transmitted to humans as well as dogs, horses and other domesticated animals by the bite of infected ticks. The causative agent B. burgdorferi was first identified in 1982 by Willy Burgdorfer, a tick-borne disease expert at Rocky Mountain Labs in Hamilton, Montana. The disease varies widely in its presentation, which may include a rash, flu-like symptoms, neurologic, arthritic and/or cardiac manifestations. Early detection and prompt antibiotic treatment usually result in an excellent prognosis, though some patients remain symptomatic. Delayed or inadequate treatment may lead to a chronic illness that is disabling and difficult to treat. Amid great controversy over diagnosis, testing and treatment, two different standards of care for Lyme disease have emerged.
The incubation period from infection to the onset of symptoms is usually 1–2 weeks, but can be much shorter (a couple of days), or even as long as one month.
The late symptoms of Lyme disease can appear months from infection. Fatality can occur when the spirochete enters brain fluids and causes meningitis, or due to conductivity defects in the heart.
Lyme disease is frequently misdiagnosed as multiple sclerosis, rheumatoid arthritis, fibromyalgia, chronic fatigue syndrome (CFS), or other (mainly autoimmune and neurological) diseases, which leaves the infection untreated and allows it to further penetrate the organism. Some of these conditions may be misdiagnosed as Lyme disease, although this is thought to be a rare occurance. False postive Lyme diagnosis is most commonly due to false positive serology in a subset of patients which suffer from syphillis, rhumatilogic diseases, or infectious mononucleosis. More confounding is that patients may present with Lyme Disease and a related disease such as MS. This makes diagnosis exceptionally difficult. It should be noted that this kind of misdiagnosis is the exception rather than the rule as it is widly held that Lyme Disease is underdiagnosed and undereported ranging from factors of 10 to upwards of 40. It is important to remember that chronic fatigue syndrome (CFS) is by definition a diagnosis of exclusion, meaning it would be inaccurate to say that a patient does not have Lyme because he or she has CFS. The substantial overlap in symptomatology between Lyme and CFS makes this a crucial point.
The longer the duration of tick attachment, the greater the risk of disease transmission, but, typically, for the spirochete to be transferred, the tick must be attached for a minimum of 12 hours, although, only the first part of this statement can be said to be strictly correct. (see Proper Removal of Ticks). Unfortunately only 20% of those infected with Lyme by the deer tick are aware of any tick bite, making early detection difficult in the absence of a rash. Tick bites usually go unnoticed due to the small size of the tick in its nymphal stage, as well as tick secretions that prevent the host from feeling any itch or pain from the bite.
Apart from this group of closely related genospecies, additional Borrelia species of interest include B. lonestari, a spirochete recently detected in the Amblyomma americanum tick (Lone Star tick) in the U.S. B. lonestari is suspected of causing STARI (Southern Tick-Associated Rash Illness), also known as Masters disease in honor of its discoverer. The illness follows a Lone Star tick bite and clinically resembles Lyme disease, but sufferers usually test negative for Lyme. There is currently no diagnostic test available for STARI/Masters, and no official treatment protocol, though antibiotics are generally prescribed. The B. miyamotoi spirochete, related to the relapsing fever group of spirochetes, is also suspected of causing illness in Japan. Spirochetes similar to B. miyamotoi have recently been found in both I. ricinus ticks in Sweden and I. scapularis ticks in the U.S.
Like other spirochetes such as T. pallidum (the agent of syphilis), B. burgdorferi has an axial filament composed of flagella which run lengthways between its cell wall and outer membrane. This structure allows the spirochete to move efficiently in corkscrew fashion through viscous media, such as connective tissue. As a result, B. burgdorferi can disseminate throughout the body within days to weeks of infection, penetrating deeply into tissue where the immune system and antibiotics may not be able to eradicate the infection.
B. burgdorferi is very slow growing, with a doubling time of 12-24 hours (in contrast to pathogens such as Streptococcus and Staphylococcus, which have a doubling time of 20-30 minutes). Since most antibiotics kill bacteria only when they are dividing, this longer doubling time necessitates the use of relatively longer treatment courses for Lyme disease. Antibiotics are most effective during the growth phase, which for B. burgdorferi occurs in four-week cycles. Some clinicians have observed that chronic Lyme patients commonly experience a worsening of symptoms every four weeks; these periodic flare-ups are thought to correspond to the growth phase of B. burgdorferi.
Various survival strategies of B. burgdorferi have been posited to explain this phenomenon, including the following:
The EM rash, which does not occur in all cases, is considered sufficient to make a diagnosis of Lyme disease and prompt treatment without further testing. In fact because of the undisputed high rate of false negatives during the early stage of the disease (before a sufficient antibody response has been established), it is recommended that tests not be performed when a patient has an EM rash.
The serological laboratory tests available are the Western blot and ELISA. In the two-tiered protocol recommended by the CDC according to their case definition, the ELISA is performed first, and if it is positive or equivocal, a Western blot is then performed to support the diagnosis. The reliability of testing in diagnosis remains controversial (see The Lyme controversy--Testing).
False-positive results for the Western blot IgM are described with varicella-zoster virus, Epstein-Barr virus, cytomegalovirus. and herpes simplex type virus 2. However studies show the Western blot IgM has a specificity of 94-96% for patients with symptoms suggestive of Lyme disease.
False-negative test results have been widely reported in both early and late disease.
Polymerase chain reaction (PCR) tests for Lyme disease may also be available to the patient. A PCR test attempts to detect the genetic material (DNA) of the Lyme disease spirochete, whereas the Western blot and ELISA tests look for antibodies to the organism. PCR tests are rarely susceptible to false-positive results but can often show false-negative results.
Lyme disease is a mimic, and as one can see from the list of symptoms, can imitate other diseases very easily. The Lyme spirochete can cross the blood-brain barrier and affect the CNS and the brain, which is very hard to treat without antibiotics that cross the barrier as well.
Given the testing difficulties described above, some patients are employing a vitamin D metabolites test as an alternative indicator. A finding of a low 25D level coupled with a high 1,25D level can be associated with an infection by B. burgdorferi or other spirochetal bacteria. Since such abnormal vitamin D levels can also be caused by other disease processes, further evaluation is warranted to rule those out before initiating treatment
Patients with chronic Lyme disease have been shown to experience a level of physical disability equivalent to that seen in congestive heart failure. The disease is rarely fatal in and of itself, although deaths have been reported.
Chronic or late diagnosed Lyme is often treated with IV antibiotics, frequently ceftriaxone, for a minimum of four weeks. As it is thought to inhibit the once-per-month breeding cycle of borrelia burgdorferi, a longer course is recommended.
With little research conducted specifically on chronic Lyme disease, treatment remains controversial. Currently there are two sets of peer-reviewed published guidelines; one advocates extended courses of antibiotics for chronic Lyme patients, while the other recommends no treatment (see The Lyme controversy--Two standards of care). Double-blind, placebo-controlled trials of long-term antibiotics for chronic Lyme have produced mixed results (see The Lyme controversy--Long-term antibiotic therapy).
Many alternative (or supplemental) therapies have been suggested. Clinical trials of large doses of IV sodium ascorbate (vitamin C) have been shown to kill cancer cells and possibly parasites in the body. Largely due to this, there are many chronic lyme disease sufferers turning to natural therapies.
It should be noted that the most important factor in treating lyme disease is finding a doctor that is familiar with the disease and all of the possible treatments. Some experts, such as Dr. Joseph J. Burrascano recommend both (sometimes long-term) IV treatment and a cocktail of various vitamins.
On one side are those who believe that Lyme disease is relatively rare, easily diagnosed with available blood tests, and easily treated with two to four weeks of antibiotics. On the other side are those who believe that Lyme disease is under-diagnosed, that available blood tests are unreliable, and that extended antibiotic treatment is often necessary. The majority of public health agencies such as the U.S. Centers for Disease Control maintain the former position, and recommend adherence to the IDSA guidelines. While this narrower position is sometimes described as the "mainstream" view of Lyme disease, physician surveys suggest otherwise. Studies show that physicians practicing in endemic areas in the U.S. are evenly split in their views, with the majority recognizing seronegative Lyme disease, and roughly half prescribing extended courses of antibiotics for chronic Lyme disease.
| View 1 | View 2 | |
| ILADS (The International Lyme and Associated Diseases Society) | IDSA (The Infectious Diseases Society of America) | |
|---|---|---|
| Peer-reviewed, published treatment guidelines | ILADS Guidelines (full text) | IDSA Guidelines (pdf) |
| EM rash | Present less than 50% of the time. Studies that show otherwise are flawed because they rely on circular logic, as subjects must meet CDC criteria which prioritize the rash over other disease manifestations. Among those who would be excluded from such studies are: 1) seronegative Lyme patients without a rash (even if there is definitive evidence of infection such as a positive PCR), 2) seropositive patients without a rash who present with fever, flu-like symptoms, joint and muscle pain, paresthesias and/or encephalopathy (symptoms not included in the restrictive CDC case definition), and 3) late-stage patients whose diagnosis was delayed because no rash was present. The exclusion of these groups leads to an artificially high estimate of the incidence of EM rash among those infected with Lyme. | "The great majority of Lyme patients" present with an EM rash, according to studies of patients with early Lyme disease diagnosed by CDC criteria. |
| Testing | Not reliable, particularly for late cases; used to support a clinical diagnosis (see Testing section for discussion). | Nearly always reliable after the first few weeks of infection. |
| Chronic Lyme disease | Persistent Lyme infection exists due to various mechanisms of antibiotic resistance, particularly when diagnosis and treatment are delayed, as numerous studies have demonstrated (see Mechanisms of persistence section). Lengthy treatment regimens are sometimes required. | Persistent Lyme infection is extremely rare. If symptoms remain after a standard course of antibiotics (several weeks), the illness becomes "Post-Lyme disease syndrome." Remaining symptoms are often attributed to an unspecified autoimmune process and/or the development of fibromyalgia or chronic fatigue syndrome, psychiatric disorders such as somatization, or simply stress. |
| Long-term antibiotic treatment | ILADS advocates long-term antibiotic therapy for symptomatic patients, while acknowledging the lack of published data supporting either long-term or short-term treatment durations. The medical literature provides a compelling rationale for the use of longer regimens for some patients. While more research is needed, treatment should not be withheld from patients in the meantime. (See Evidence section for list of published clinical trials.) | The IDSA does not recommend long-term antibiotic therapy for patients with chronic Lyme disease because of a lack of published data supporting its use. (See Evidence section for list of published clinical trials.) |
| Primary concern regarding misdiagnosis | The under-diagnosis of Lyme may lead to untreated chronic, persistent infection resulting in severe disability and possibly even death. | The over-diagnosis of Lyme may lead to the unnecessary use of antibiotics resulting in side effects (most commonly nausea), and rarely, complications from intravenous antibiotics. There are also concerns about the cost of antibiotic treatment. |
| Risk-benefit analysis | The potential harm in letting a persistent Lyme infection go untreated far outweighs the potential side-effects of long-term antibiotic use. This therapy is generally safe when administered by skilled clinicians who take appropriate precautions. If it is considered safe enough for acne patients, its use is certainly justified for chronic Lyme patients. | Since chronic Lyme infection is presumed not to exist, any potential adverse effects of long-term antibiotic therapy outweigh the (non-existent) benefits. |
A number of well-documented signs of chronic Lyme disease including encephalopathy (manifested by memory loss, mood changes and sleep disturbance) are not part of the CDC case definition. Therefore clinicians using the CDC criteria for diagnostic purposes will misdiagnose patients who have the disease. Additionally, reliance on the CDC case definition for clinical purposes would result in the misdiagnosis of those with false-negative test results, a widely reported phenomenon (see Diagnosis).
There is little concrete evidence either for or against the use of antibiotics for chronic Lyme disease, because only three such double-blind, placebo-controlled clinical trials have been funded to date by the U.S. National Institutes of Health, with conflicting results.
1) Klempner et al (2001). One month of intravenous ceftriaxone followed by two months of low-dose oral doxycycline (or placebo) given to chronic Lyme patients with one or more of the following symptoms: musculoskeletal pain, cognitive impairment, radicular pain, paresthesias or dysesthesias.
2) Krupp et al (2003). Four weeks of intravenous ceftriaxone or placebo given to chronic Lyme patients with "persistent severe fatigue".
3) Fallon et al (not yet published). Results presented on October 22, 2004 at the Columbia University/Lyme Disease Association Conference in Rye, NY (Press release). Ten weeks of intravenous ceftriaxone or placebo given to chronic Lyme patients with ongoing memory impairment.
It is important to note that Fallon et al's study is the only biological examination of Chronic Lyme Disease to date. In the two other studies, results were interpreted using questionaires, often administered over the phone.
Fallon's study had several blinds. This level of methodology has never before been attempted in a study of Chronic Lyme Disease. One of the reasons that many levels of blind were used in Fallon's study has to do with the controvery sourounding Lyme Disease. The aim of this study was to include people for whom there was little dissagreement in terms of a correct Lyme Disease Diagnosis. Secondly, the strict methodology, though tedious, was required because scientific rigor of a very high degree was neccesary given the political nature of Lyme Disease. In this study, patients with Chronic Lyme Disease were given SPEC Scans before and after treatment. A SPEC scan is a scan of the brain which qualitativly or quantitavily (depending on the sophistication of the equiptment) measures metabolic and blood flow activity within the brain. This is a physical marker that can scientifically examine cause and effect as opposed to questionaires which are open to the opinions of the participant and influence of the examinor. Patients were also administered purly quantititative examinations aimed at assesing disabilty, ie: nueropychological testing. Lastly, as in other studies, patients were asked how they felt after treatment. All of these tests included several degrees of blind, ie: radiologist blind to diagnosis, nueropychiatrists blind to diagnosis, patient blind to treatment, ect..
A method of protecting your whole property - Damminix - is also cited. It consists of biodegradable cardboard tubes stuffed with permethrin-treated cotton and works in the following way: Mice collect the cotton for lining their nests. The pesticide on the cotton kills any immature ticks that are feeding on the mice. It is important to put the tubes where mice will find them, such as in dense, dark brush or at the base of a log; mice are unlikely to gather the cotton from an open lawn. Best results are obtained with regular applications early in the spring and again in late summer. The more neighbors who also use Damminix, the better. Damminix appears to help control tick populations, particularly in the year following initial use. Note that it is not effective on the West Coast. Protecting Property from Tick Infestation: Damminix * University of Maryland Medical Center
A potential alternative to Damminix, the Maxforce Tick Management system, is based on plastic baitboxes that attract rodents. Rodents entering these baitboxes would then be painted with fipronil. This product requires professional installation. As of June 2006, this product is no longer available. (http://www.maxforcetms.com). The reason appears to have been that in 2005, there were selective reports of grey squirrels "chewing" into some Maxforce TMS boxes in areas of the northeastern United States, compromising the child resistant box. Due to this problem, the Federal Environmental Protection Agency (EPA) has asked that all similarly designed TMS boxes applied in 2006 be covered with a protective shroud capable of preventing squirrel damage (http://www.maxforcetmspro.com/).
A vaccine against a North American strain of the spirochetal bacteria was available between 1998 and 2002. When taking it off the market, the manufacturer cited poor sales, though some people believe that the actual reason was that the vaccine was not safe or effective at all.Safety/Efficacy concerns re: Lyme vaccine: LYMErix Controversy LymeInfo.net
The advice of the UK's Hospital for Tropical Diseases is that significant exposure (an attached mite for more than twelve hours) should be managed, as in America & Germany, with Doxycycline 100 mg twice a day for three days.Antibiotic Prophylaxis After Tick Bite For Prevention Of Lyme Disease An Annotated Bibliography Patients should be advised to report any Erythema migrans over the subsequent two to six weeks. If there should be suspicion of disease, then a course of Doxycycline should be immediately given for ten days; without awaiting serology tests which only yield positive results after an interval of one to two months.
The deer tick (Ixodes scapularis, the primary vector in the northeastern U.S.) has a two-year life cycle, first progressing from larva to nymph, and then from nymph to adult. The tick feeds only once at each stage. In the fall, large acorn forests attract deer as well as mice, chipmunks and other small rodents infected with B. burgdorferi. During the following spring, the ticks lay their eggs. The rodent population then "booms." Tick eggs hatch into larvae, which feed on the rodents; thus the larvae acquire infection from the rodents. (Note: At this stage, it is proposed that tick infestation may be controlled using acaricides (miticide). A commercial method is to provide nesting material soaked in permethrin (Damminix).) The infected larvae molt into nymphs. These infected nymphs transmit the majority of Lyme infection to humans, feeding on humans and small animals from spring through summer. The nymphs then molt into adults, which feed on larger animals such as deer in the fall and early spring. Adult ticks may also transmit disease to humans. After feeding, female adult ticks lay their eggs on the ground, and the cycle is complete. Note: on the west coast, Lyme disease is spread by the western black-legged tick (Ixodes pacificus), which has a different life cycle.
The disease was first documented as a skin rash in Europe in 1883. Over the years, researchers there identified additional features of the disease, including an unidentified pathogen, its response to penicillin, the role of the Ixodes tick (black legged tick) as its vector, and other symptoms including those affecting the central nervous system.
In the U.S., Borrelia burgdorferi has been isolated in the skin of white-footed mice in museum specimens that date back to the 1870s in Massachusetts, but researchers were unaware of the organism's existence until the 1970s. Interest in tick-borne infections in the U.S. began with the first report of tick-borne relapsing fever in 1905, and the discovery of the wood tick's role as a vector of Rocky Mountain spotted fever the following year. However, the full syndrome now known as Lyme disease was not recognized until a cluster of cases originally thought to be juvenile rheumatoid arthritis was identified in three towns in southeastern Connecticut in 1977. Two of these towns, Lyme and Old Lyme, gave the disease its popular name.
In 1982 a novel spirochete was isolated and cultured from the midgut of Ixodes ticks, and subsequently from patients with Lyme disease. The infecting agent was first identified by Jorge Benach, and soon after isolated by Willy Burgdorfer, a scientist at the National Institutes of Health, who specialized in the study of spirochete microorganisms. The spirochete was named Borrelia burgdorferi in his honor. Burgdorfer was the partner in the successful effort to culture the spirochete, along with Alan Barbour.
Infectious diseases | Zoonoses | Bacterial diseases
Lymeská borelióza | Borreliose | Lyme-Borreliose | Enfermedad de Lyme | Borrelioosi | Borréliose | ライム病 | Lyme-ziekte | Borelioza | Doença de Lyme | Lymská borelióza | Borrelia | Må d' Lyme | 莱姆病
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