User:Eliška Koutná/Sandbox 3

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The vCJD form was described for the first time during the BSE epidemic in the United Kingdom in 1996 and was termed as the “new variant CJD” <ref>PMID 8598754</ref>. It is primarily caused by ingestion of food with infectious contamination originating from BSE affected cattle <ref>DOI 10.1002/ana.20708</ref>. Nonetheless, infection can also arise from transfusion by an infected blood <ref>DOI 10.1111/vox.12371</ref> or a blood product, i.e. factor VIII important in the pathway of the blood coagulation <ref>DOI 10.1111/j.1365-2516.2009.02181.x</ref>. The BSE epidemic is the main reason for which the vCJD still occurs with highest incidence in the UK and France. Since 1996 till 25.04.2017, total count of 231 definite or probable cases of vCJD was reported <ref name="knight" />. Symptoms of vCJD are again mostly identical or very similar to those of other CJD forms, including painful sensory symptoms and involuntary movements <ref>DOI 10.1002/ana.21987</ref>. In compare with sCJD, mean survival of patients from the onset symptoms is significantly longer, approximately 14 months from the onset symptoms <ref>DOI 10.1136/jnnp.2010.232264</ref>.
The vCJD form was described for the first time during the BSE epidemic in the United Kingdom in 1996 and was termed as the “new variant CJD” <ref>PMID 8598754</ref>. It is primarily caused by ingestion of food with infectious contamination originating from BSE affected cattle <ref>DOI 10.1002/ana.20708</ref>. Nonetheless, infection can also arise from transfusion by an infected blood <ref>DOI 10.1111/vox.12371</ref> or a blood product, i.e. factor VIII important in the pathway of the blood coagulation <ref>DOI 10.1111/j.1365-2516.2009.02181.x</ref>. The BSE epidemic is the main reason for which the vCJD still occurs with highest incidence in the UK and France. Since 1996 till 25.04.2017, total count of 231 definite or probable cases of vCJD was reported <ref name="knight" />. Symptoms of vCJD are again mostly identical or very similar to those of other CJD forms, including painful sensory symptoms and involuntary movements <ref>DOI 10.1002/ana.21987</ref>. In compare with sCJD, mean survival of patients from the onset symptoms is significantly longer, approximately 14 months from the onset symptoms <ref>DOI 10.1136/jnnp.2010.232264</ref>.
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The susceptibility to infection and disease, incubation period and duration of survival in all CJD forms are dependent on several different factors including age of onset and genetic predispositions. So called PRNP-129 polymorphism is related to all CJD forms, but especially to iCJD. Its principle lies in genotype combinations of Met129 and Val129 alleles (MM, MV or VV) and in iCJD, it has substantial impact on susceptibility and incubation period of the disease caused by infection from previously mentioned treatment with hGH <ref name="brandel">DOI 10.1016/S0140-6736(03)13867-6</ref>. It appears that VV and mainly MM homozygotes are more susceptible to infection by CJD and have shorter incubation period than MV heterozygotes <ref name="brandel" /><ref name="parchi">PMID 10443888</ref>. Furthermore, supporting this hypothesis almost all definite and probable vCJD and sCJD reported cases are of MM genotype <ref name="parchi" /><ref>DOI 10.1016/S0140-6736(09)61568-3</ref>.
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The susceptibility to infection and disease, incubation period and duration of survival in all CJD forms are dependent on several different factors including age of onset and genetic predispositions. So called PRNP-129 polymorphism is related to all CJD forms, but especially to iCJD. Its principle lies in genotype combinations of Met129 and Val129 alleles (MM, MV or VV) and in iCJD, it has substantial impact on susceptibility and incubation period of the disease caused by infection from previously mentioned treatment with hGH <ref name="brandel">DOI 10.1016/S0140-6736(03)13867-6</ref>. It appears that VV and mainly MM homozygotes are more susceptible to infection by CJD and have shorter incubation period than MV heterozygotes <ref name="brandel" /><ref name="parchi">PMID 10443888</ref>. Furthermore, supporting this hypothesis almost all definite and probable vCJD and sCJD reported cases are of MM genotype <ref name="parchi" /><ref>PMID 20109837</ref>.
== '''Diagnosis and treatment''' ==
== '''Diagnosis and treatment''' ==

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