JM2, encoding a fork head–related protein, is mutated in X-linked autoimmunity–allergic disregulation syndrome
Talal A. Chatila, … , Cindy Helms, Anne M. Bowcock
Talal A. Chatila, … , Cindy Helms, Anne M. Bowcock
Published December 15, 2000
Citation Information: J Clin Invest. 2000;106(12):R75-R81. https://doi.org/10.1172/JCI11679.
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JM2, encoding a fork head–related protein, is mutated in X-linked autoimmunity–allergic disregulation syndrome

Abstract

X-linked autoimmunity–allergic disregulation syndrome (XLAAD) is an X-linked recessive immunological disorder characterized by multisystem autoimmunity, particularly early-onset type 1 diabetes mellitus, associated with manifestations of severe atopy including eczema, food allergy, and eosinophilic inflammation. Consistent with the allergic phenotype, analysis of two kindreds with XLAAD revealed marked skewing of patient T lymphocytes toward the Th2 phenotype. Using a positional-candidate approach, we have identified in both kindreds mutations in JM2, a gene on Xp11.23 that encodes a fork head domain–containing protein. One point mutation at a splice junction site results in transcripts that encode a truncated protein lacking the fork head homology domain. The other mutation involves an in-frame, 3-bp deletion that is predicted to impair the function of a leucine zipper dimerization domain. Our results point to a critical role for JM2 in self tolerance and Th cell differentiation.

Authors

Talal A. Chatila, Frank Blaeser, Nga Ho, Howard M. Lederman, Constantine Voulgaropoulos, Cindy Helms, Anne M. Bowcock

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Figure 1

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Haplotype analysis of pedigrees XLAAD-100 and XLAAD-200. Circles, female...
Haplotype analysis of pedigrees XLAAD-100 and XLAAD-200. Circles, females; squares, males. Filled symbols, affected individuals; open symbols, unaffected individuals; forward slash through symbol, deceased individual. X chromosome haplotypes are schematically represented by side bars, while numbers next to the side bars represent the sizes (in bp) of alleles of markers listed in the inset. XLAAD-200-16, -17, -18, and -29 died of fetal hydrops. A question mark refers to deceased males whose genotype could not be determined. Haplotypes for X chromosome markers are shown. A crossover proximal to marker DXS1068 in individual XLAAD-200-4 defines DXS1223 as the proximal flanking marker for XLAAD, and a second recombination in XLAAD-200-27 distal to DXS6800 defines DXS6789 as the distal flanking marker for the XLAAD locus.