AI Article Synopsis
- - X-linked severe combined immunodeficiency (XSCID) is typically due to mutations in the common gamma chain, which leads to a lack of T and natural killer (NK) cells.
- - An unusual case of XSCID showed the presence of functional T and NK cells along with symptoms similar to Omenn syndrome, due to a specific splice-site mutation that allowed some normal gammac expression.
- - The patient's skin biopsy revealed a significant presence of revertant T cells with a second mutation that corrected splicing issues, suggesting that XSCID can present in unexpected ways and that genetic mosaicism plays a role in diverse clinical outcomes.
Article Abstract
X-linked severe combined immunodeficiency (XSCID) is caused by mutations of the common gamma chain (gammac) and usually characterized by the absence of T and natural killer (NK) cells. Here, we report an atypical case of XSCID presenting with autologous T and NK cells and Omenn syndrome-like manifestations. The patient carried a splice-site mutation (IVS1+5G>A) that caused most of the mRNA to be incorrectly spliced but produced normally spliced transcript in lesser amount, leading to residual gammac expression and development of T and NK cells. The skin biopsy specimen showed massive infiltration of revertant T cells. Those T cells were found to have a second-site mutation and result in complete restoration of correct splicing. These findings suggest that the clinical spectrum of XSCID is quite broad and includes atypical cases mimicking Omenn syndrome, and highlight the importance of revertant mosaicism as a possible cause for variable phenotypic expression.
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| http://dx.doi.org/10.1182/blood-2008-04-149708 | DOI Listing |
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