Journal
HUMAN GENETICS
Volume 119, Issue 3, Pages 284-294Publisher
SPRINGER
DOI: 10.1007/s00439-006-0138-9
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Funding
- Intramural NIH HHS Funding Source: Medline
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Autoimmune lymphoproliferative syndrome (ALPS) is characterized by lymphadenopathy, elevated numbers of T cells with alpha beta-T cell receptors but neither CD4 nor CD8 co-receptors, and impaired lymphocyte apoptosis in vitro. Defects in the Fas receptor are the most common cause of ALPS (ALPS Ia), but in rare cases other apoptosis proteins have been implicated, including caspase-10 (ALPS II). We investigated the role of variants of caspase-10 in ALPS. Of 32 unrelated probands with ALPS who did not have Fas defects, two were heterozygous for the caspase-10 missense mutation 1406L. Like the previously reported ALPS II-associated mutation L285F, I406L impaired apoptosis when transfected alone and dominantly inhibited apoptosis mediated by wild type caspase-10 in a co-transfection assay. Other variants in caspase-10, V410I and Y446C, were found in 3.4 and 1.6% of chromosomes in Caucasians, and in 0.5 and < 0.5% of African Americans, respectively. In contrast to L285F and 1406L, these variants had no dominant negative effect in co-transfection assays into the H9 lymphocytic cell line. We found healthy individuals homozygous for V410I, challenging the earlier suggestion that homozygosity for V4101 alone causes ALPS. Moreover, an association analysis suggested protection from severe disease by caspase-10 V4101 in 63 families with ALPS la due to dominant Fas mutations (P < 0.05). Thus, different genetic variations in caspase-10 can produce contrasting phenotypic effects.
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