The following are questions and answers regarding the XMRV retro-virus. Contact us if you have a question you'd like answered. Select from the table below for more FAQ's.

• Who were the patients & healthy controls in the recent XMRV study published in Science?
• Would having other details about the patients impact the ability of others to replicate this work?
• What is XMRV?
• What is the link between XMRV and CFS/ME, fibromyalgia and other neuro-immune diseases?
• Where can I get tested for XMRV?
• How is XMRV transmitted?
• Is XMRV airborne?
• What does it mean if I am infected with XMRV?
• How do I volunteer for clinical trials or other research?
• Why was XMRV looked for in neuro-immune diseases?
• Where did the Whittemore Peterson Institute get the blood samples used for this study?
• Can you catch CFS/ME?
• If I am pregnant or thinking about getting pregnant and have CFS/ME, should I be concerned about protecting my unborn child?
• What can my doctor do for me if I test positive to the XMRV virus?
• Are there federal guidelines for dealing with XMRV?
• Who discovered XMRV?
• How many retroviruses are there?
• I have been diagnosed with CFS/ME and recently tested positive for XMRV. My friends and family ask that if I am sick and have a retrovirus, why do I look normal?
• Most thought CFS/ME was a woman's disease. But XMRV has been found in men with prostate cancer and now people with CFS/ME. What does this say about CFS/ME?
• Does this latest information prove once and for all that CFS/ME is not a psychological or psychosomatic illness as described by those who don't understand the disease?
• Is XMRV only in the United States or is it elsewhere?

Every patient sample used in the study (taken from the nationwide WPI repository gathered from several regional physician practices) had a physician's diagnosis of CFS. To further validate the samples, the research team used the well-established CDC and Canadian Consensus Criteria for CFS in every case. The healthy controls were healthy people who came to a doctor's office for a routine sample or from DNA used in routine diagnostics.

In order to meet legal human assurance requirements, identifiers for the control population are not available to the investigators. Nor was additional information on the patient samples used in this study. Age, sex, duration of illness, medical history and medication use have no impact on the identification of a new human retroviral pathogen.

No, but one must have the appropriate testing methods and tools to replicate. Retroviruses do not discriminate based on age, sex or any other characteristic listed. Additionally, because the healthy controls were zip code matched, as well as age and sex matched, no further information on the controls is needed.

These CFS patients have a diagnosis of CFS as described by the Canadian Consensus and CDC definitions. There is nothing unique about these patients. In this research 67% of the study group had an active infectious retrovirus in their blood versus 3.75% of the healthy controls.

The scientists who refereed this paper concluded that we met every scientific and clinical criterion with the rigor required by a journal with the highest standards in the world. Science and its referees understand the importance of the finding that a new human retrovirus is infectious and transmissible and highly associated with CFS.

Future research will look at prevalence among population groups, transmissibility, interaction with medications, impact of the duration of a CFS diagnosis on the activity of XMRV, and a wide variety of other factors. We are all interested in these results, as well as treatments studies to determine best management of infections.

This is a very serious public health concern: 3.75% of the healthy controls (which would translate to 10 million Americans) in this study were infected with a newly described retrovirus of unknown pathogenic potential.

Researchers at the Whittemore Peterson Institute in collaboration with the National Cancer Institute and the Cleveland Clinic, have recently discovered the presence of a retrovirus in blood samples from patients diagnosed with chronic ME/ CFS. The human retrovirus, identified as XMRV, has now been found to be in over 95 percent of the patients' blood samples in this study group.

XMRV is a human retrovirus and is similar to HIV and HTLV-1. It was first identified by Dr. Robert Silverman, in prostate cancer tissue of men with a specific genetic defect in their antiviral defense pathway. Prior to the Whittemore Peterson Institute study, XMRV had not been isolated from a human diseased population or been shown to be infectious and transmissible.

The initial research showed that 67% of the CFS/ME patient samples tested positive for XMRV. Further work has found that 95% tested positive. Work continues to understand how this virus works within neuro-immune diseases, but this discovery proves a significant correlation between this serious retrovirus and these diseases. Our work suggests, but does not prove, that XMRV may be the underlying cause of CFS/ME. Much additional work needs to be done to understand how XMRV causes disease and what types of diseases it is linked to it.

A few fibromyalgia samples were tested and yes, they were positive. However the sampling was very small, and testing will have to continue on a much larger scale to begin to draw significant conclusions. In addition, many patients with CFS/ME have been given the diagnosis of fibromyalgia when in fact they have CFS/ME and fibromyalgia.

The Whittemore Peterson Institute (WPI) is now allowing Viral Immune Pathology Diagnostics (VIP Dx) to temporarily offer the tests researchers used in the study linking XMRV to chronic fatigue syndrome (CFS/ME). Viral Immune Pathology Diagnostics (VIP Dx), in Reno, NV, which is also where the WPI is located. The institute says net proceeds from the test will be dedicated to further research.

For more information about the test kit, go to the VIP Dx website. At this time, this is the only lab test associated with the WPI research, although many companies are advertising XMRV tests online.

XMRV is thought to be transmitted through body fluids such as blood, semen, and mother's breast milk but is not transmitted through the air. It is not known whether XMRV is more easily transmitted than other human retroviruses.

No, retroviruses are not traditionally airborne viruses. However, since XMRV is a blood borne retrovirus, it may be possible to transmit through sexual contact, sharing needles, blood transfusions, and breastfeeding. Sharing household items like toothbrushes, razors, or items that come into contact with blood is not recommended as a precautionary measure.

The research continues to fully understand the connection between CFS/ME and XMRV, as well as what it means to have the virus. We do not know all of the health ramifications of XMRV or CFS/ME, but we do know that some people with CFS/ME, have on average a lower life expectancy than someone without this chronic disease. In other studies XMRV has been detected in very aggressive cancerous prostate tumors. One may have XMRV and not have CFS/ME as evidenced by positive results of 3.7 percent of our control samples.

If you are interested in possibly being selected to participate in ongoing or future Whittemore Peterson Institute (WPI) research studies visit their website and fill out the WPI Volunteer Questionnaire. While every study has specific requirements and not all who volunteer will be accepted, your willingness to participate is both crucial and deeply appreciated.

Patients who have been diagnosed with CFS/ME have been shown to have a unique immune deficiency in a part of their antiviral system called the RNase L pathway. This pathway was also deficient in men whose cancer samples were first used in the discovery of XMRV. In this study, however, Whittemore Peterson Institute researchers have found XMRV in patients without an RNase L pathway deficiency. It is not known if XMRV causes this deficiency or if patients with this deficiency are more susceptible to the virus' effects or both.

The blood samples used in this historic study were collected from several different regions within the United States and included both a known CFS/ME population and a control group. Of those diagnosed with CFS/ME, over 95 percent have recently been found to have antibodies to XMRV in their blood.

Causation of CFS/ME is likely to be a multi-factorial process which occurs in a susceptible person with common viral co-infections. CFS/ME is a complex, systemic neuro-immune disease that is estimated to affect over one million Americans and 17 million people worldwide. CFS/ME has traditionally been diagnosed by the exclusion of other similarly presenting conditions, such as MS and lupus, and by a series of symptoms; making the diagnosis an expensive and difficult process. Until now, a single viral link (while suspected by many) had not been made because so many common viruses have been found to be reactivated in persons with CFS/ME. This finding suggests a role for XMRV in the pathogenesis of CFS/ME and creates a better understanding of the disease. Our work suggests but does not prove that XMRV may be the underlying cause of CFS/ME. Much additional work needs to be done to understand how XMRV causes disease and what types of diseases it is linked to it.

As a CFS/ME patient who is either pregnant or thinking about getting pregnant, you should speak with your physician regarding XMRV and safety measures you can use to minimize possible transmission of this virus to your child.

Research is still ongoing to determine the best treatments for those who are positive for XMRV. It is possible that antiviral therapies developed for other retroviruses may be useful against another RNA virus like XMRV. However, these are generally toxic therapies with considerable side effects making it imperative that one be very careful before beginning any new therapies. Obviously, only begin any therapies approved by your physician.

Guidelines will be established as more is leaned about XMRV.

XMRV was originally discovered in prostate cancer tumors by Dr. Robert Silverman. Scientists from the Whittemore Peterson Institute, Cleveland Clinic and the National Cancer Institute were the first to discover XMRV in the blood of Chronic Fatigue Syndrome/Myalgic Encephalomyelitis (CFS/ME) patients.

Currently there are only three known infectious human retroviruses; HIV, HTLV-1 and 2 and now XMRV. HIV causes AIDS and HTLV-1 and 2 causes T-cell leukemia and T-cell lymphoma. XMRV is the most recent retrovirus discovered to infect humans and has been linked to neurological disease and prostate cancer.

Like other retroviruses known to infect humans, these illnesses appear to be invisible to the untrained eye. A physician, however, can see the signs of illness, and still must carefully examine the patient to know for certain who is ill and with what disease. Many diseases fall into this category. Unless one develops a disease that creates physical lesions that people can see e.g. psoriasis, the mask of lupus or the crippling bone changes of arthritis, most people can not see how debilitating the illness actually is. In addition, each person responds differently to treatment and therefore can maintain a higher quality of health and appearance of health. In the case of HIV, many people are infected but do not appear to be ill.

CFS/ME is not a woman's disease. In fact the epidemiological study done by Dr. Lenny Jason has shown that this disease occurs in men and women and is also prevalent in children. Instances of outbreaks in which entire families and groups of friends became ill near the same time, have been reported across the US, the UK and other countries.

Absolutely! Actually, there are thousands of research articles showing the very real biological problems that CFS/ME patient's experience such as low NK cell count and function, MRI and SPEC scan changes, and repeated chronic infections, to mention just a few. Only the most stubborn and misinformed individuals refuse to believe that this disease is real and serious. The process of placing poorly understood illnesses into a psychological category is very similar to what happened in the early days of MS and epilepsy before the advent of technologies which proved the illnesses were "real." Unfortunately, many in the scientific and medical fields have not learned from their past mistakes.

For the purposes of this study, samples were collected from many different areas within the United States. However, as with other retroviruses, there is no reason to believe that the virus is not present in all other parts of the world.

• More Articles About XMRV Virus Discovery