Fred C. Westall scite author profile

A highly encephalitogenic peptide whose structure resembles the sequence of amino acids surrounding the single tryptophan residue in the encephalitogenic A1 protein from bovine myelin was synthesized. This peptide is similar in the sequence to peptic peptide E and tryptic T27, derived directly from the A1 protein, and is as active on a molar basis as the A1 protein. The major disease-inducing site of the A1 protein resides in a linear sequence of nine amino acids: H-Phe-Ser-Trp-Gly-Ala-Glu-Gly-Gln-Lys-OH. This region of the A1 protein is apparently the major encephalitogenic determinant since specific modification of the tryptophan residue in the A1 protein with 2-hydroxy-5-nitrobenzyl bromide destroyed its encephalitogenic activity.

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Molecular Mimicry Revisited: Gut Bacteria and Multiple Sclerosis

Westall¹

2006

J Clin Microbiol

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Molecular mimicry is a possible explanation for autoimmune side effects of microorganism infections. Protein sequences from a particular microorganism are compared to known autoimmune immunogens. For diseases such as multiple sclerosis (MS), where the infectious agent is unknown, guesses to its identity are made. Mimics are assumed to be rare. This study takes a radically different approach. Reported sequences from all known human bacterial and viral agents were searched for autoimmune immunogen mimics. Three encephalitogenic peptides, whose autoimmune requirements have been studied extensively, were selected for comparison. Mimics were seen in a wide variety of organisms. For each immunogen, the mimics were found predominantly in nonpathogenic gut bacteria. Since the three immunogens used in this study are related to MS, it is suggested that a microorganism responsible for autoimmune activity in MS could be a normally occurring gut bacterium. This would explain many of the peculiar MS epidemiological data and why no infective agent has been identified for MS and supports recently found MS gut metabolism abnormalities.

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Essential Chemical Requirements for Induction of Allergic Encephalomyelitis

Westall

Robinson

Caccam

et al. 1971

Nature

189

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Brain-derived fibroblast growth factor: A study of its inactivation

1983

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Fred C. Westall

Experimental Allergic Encephalomyelitis: Synthesis of Disease-Inducing Site of the Basic Protein

Molecular Mimicry Revisited: Gut Bacteria and Multiple Sclerosis

Essential Chemical Requirements for Induction of Allergic Encephalomyelitis

Brain-derived fibroblast growth factor: A study of its inactivation

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