Myasthenia gravis. T epitopes on the delta subunit of human muscle acetylcholine receptor.

MP Protti, AA Manfredi, XD Wu, L Moiola… - … (Baltimore, Md.: 1950 …, 1991 - journals.aai.org
MP Protti, AA Manfredi, XD Wu, L Moiola, JF Howard Jr, BM Conti-Tronconi
Journal of immunology (Baltimore, Md.: 1950), 1991journals.aai.org
Autoimmune T cell lines specific for muscle nicotinic acetylcholine receptor (AChR) were
propagated from the blood of three myasthenia gravis patients by the use of a pool of
synthetic peptides (delta-pool) corresponding to the complete sequence of the delta-subunit
of human muscle AChR. Propagation of AChR-specific T cell lines was attempted
unsuccessfully from four other myasthenia gravis patients and from four healthy controls.
The lines had CD3+, CD4+, CD8-phenotype, strongly recognized the delta-pool, and cross …
Abstract
Autoimmune T cell lines specific for muscle nicotinic acetylcholine receptor (AChR) were propagated from the blood of three myasthenia gravis patients by the use of a pool of synthetic peptides (delta-pool) corresponding to the complete sequence of the delta-subunit of human muscle AChR. Propagation of AChR-specific T cell lines was attempted unsuccessfully from four other myasthenia gravis patients and from four healthy controls. The lines had CD3+, CD4+, CD8- phenotype, strongly recognized the delta-pool, and cross-reacted vigorously with non-denatured AChR purified from mammalian muscle. They did not cross-react detectably with pools of similar overlapping synthetic peptides corresponding to the complete sequences of the alpha- and gamma-subunits of human muscle AChR. The sequence segments of the delta-subunit that contain T epitopes were identified by investigating the response of the three CD4+ T cell lines to the individual synthetic peptides forming the delta-pool. Each line had an individual pattern of peptide recognition. Although no immunodominant region, recognized in association with different DR haplotypes, could be identified, the sequence segments most strongly recognized by the CD4+ T cell lines were clustered within residues 121-290. One of the peptides more strongly recognized by the T cells corresponded to a sequence segment with high predicted propensity to form an amphipathic alpha-helix, a structural motif proposed to be typical of T epitopes.
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