Survey
* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project
Download document - Lymphoma Coalition
Document related concepts
Childhood immunizations in the United States wikipedia , lookup
Human leukocyte antigen wikipedia , lookup
Sociality and disease transmission wikipedia , lookup
Hygiene hypothesis wikipedia , lookup
Kawasaki disease wikipedia , lookup
Behçet's disease wikipedia , lookup
Eradication of infectious diseases wikipedia , lookup
Neuromyelitis optica wikipedia , lookup
Sjögren syndrome wikipedia , lookup
Ankylosing spondylitis wikipedia , lookup
Globalization and disease wikipedia , lookup
Germ theory of disease wikipedia , lookup
African trypanosomiasis wikipedia , lookup
Transcript
Genetic Studies of Non-Hodgkin Lymphoma With the completion of the sequencing of the human genome, much attention has been centered on the study of human genetic variability in disease risk. Single nucleotide polymorphisms (SNPs) are the most common source of human genetic variation, and they are, undoubtedly, a valuable resource for investigating the genetic basis of cancers such as lymphoma. Although the majority of these gene variants do not influence disease risk, certain SNPs may influence susceptibility to disease, disease severity, disease progression or other outcomes related to the disease. One of the biggest current challenges in biomedical research is the identification of these gene variants. In genetic epidemiology, a genome-wide association study (GWAS) is an examination of hundreds of thousands of variations, generally SNPs, in a sample population. These studies normally compare the variations of two groups of participants: people with the disease (cases) and similar people without the disease (controls). If the frequency of particular SNPs vary between the cases and controls, the variations are said to be "associated" with the disease. In our group, we are investigating how human genetic variation influences the risk of lymphoma. Using GWAS studies, we searched for variations in the genome associated with major types of non-Hodgkin lymphoma (NHL) in a group of over 1400 NHL cases and controls from the San Francisco Bay Area. We found several SNPs that were statistically significantly more frequent in follicular lymphoma cases than in the controls, and therefore are potentially involved in risk of the disease. These SNPs were mainly located in the human leukocyte antigen (HLA) region, a part of the genome that contains a large number of genes related to immune system function, and that plays an important role in several other diseases, particularly in autoimmune disorders. Further analyses of the HLA region identified additional genetic differences between the follicular lymphoma cases and controls suggesting that HLA gene variants may play an important role in disease susceptibility. Some of these HLA gene regions have also been shown to influence risk of rheumatoid arthritis and type 1 diabetes. Although these findings have been validated by other studies within the large lymphoma consortium, InterLymph, much caution must be taken when extrapolating the results. As with any other cancer, NHL is a very complex disease that arises from the interaction between multiple variations in different genes and non-genetic factors, such as environmental exposures and lifestyle. Further studies will be needed to determine how these gene-environment interactions influence disease risk.
