Alma Maciulis scite author profile

Autism likely results from several different etiologies or a combination of pathological mechanisms. Recent studies suggest that this disorder may be associated with immune abnormalities, pathogen-autoimmune processes and perhaps the major histocompatibility complex (MHC). In a preliminary study we found that 22 autistic subjects had an increased frequency of the extended or ancestral MHC haplotype B44-SC3O-DR4. The current study attempted to confirm this observation by studying 23 additional randomly chosen autistic subjects, most of their parents and 64 unrelated normal subjects. In agreement with earlier findings B44-SC3O-DR4 was associated with autism. In combining the data from the original and current studies, B44-SC3O-DR4 or a substantial fragment of this extended haplotype was represented in 40% of the autistic subjects and/or their mothers as compared to about 2% of the unrelated subjects. It is concluded that one or more genes of the MHC is (are) involved in the development of some cases of autism.

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Immunogenetic studies in autism and related disorders

Warren

Singh

Averett

et al. 1996

Molecular and Chemical Neuropathology

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The major histocompatibility complex comprises a number of genes that control the function and regulation of the immune system. One of these genes, the C4B gene, encodes a product that is involved in eliminating pathogens such as viruses and bacteria from the body. We previously reported that a deficient form of the C4B gene, termed the C4B null allele (no C4B protein produced) had an increased frequently in autism. In this study we attempted to confirm the increased incidence of the C4B null allele in autism and investigated the presence of a C4B null allele in two other childhood disorders, attention-deficit hyperactivity disorder and dyslexia (reading disability). In addition, we explored the relationship of autism to the DR beta 1 gene, a gene located close to the C4B in autism. We confirmed the finding of an increased frequency of the C4B null allele in autism and found that the related disorders also had an increased frequency of this null allele. In addition, two alleles of the DR beta 1 gene also had significantly increased representation in the autistic subjects.

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Strong association of the third hypervariable region of HLA-DRβ1 with autism

Warren

Odell

Warren

et al. 1996

Journal of Neuroimmunology

121

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Alma Maciulis

The transmission disequilibrium test suggests that HLA-DR4 and DR13 are linked to autism spectrum disorder

Confirmation of the association of the C4B null allelle in autism

Increased Frequency of the Extended or Ancestral Haplotype B44-SC3O-DR4 in Autism

Immunogenetic studies in autism and related disorders

Strong association of the third hypervariable region of HLA-DRβ1 with autism

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