Evaluation of the risk for Tay-Sachs disease in individuals of French Canadian ancestry living in New England

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Abstract

Background: The assessment of risk for Tay-Sachs disease (TSD) in individuals of French Canadian background living in New England is an important health issue. In preliminary studies of the enzyme-defined carrier frequency for TSD among Franco-Americans in New England, we found frequencies (1:53) higher than predicted from the incidence of infantile TSD in this region. We have now further evaluated the risk for TSD in the Franco-American population of New England. Methods: Using a fluorescence-based assay for β-hexosaminidase activity, we determined the carrier frequencies for TSD in 2783 Franco-Americans. DNA analysis was used to identify mutations causing enzyme deficiency in TSD carriers. Results: We determined the enzyme-defined carrier frequency for TSD as 1:65 (95% confidence interval 1:49 to 1:90). DNA-based analysis of 24 of the enzyme-defined carriers revealed 21 with sequence changes: 9 disease-causing, 4 benign, and 8 of unknown significance. Six of the unknowns were identified as c.748G > A p.G250S, a mutation we show by expression analysis to behave similarly to the previously described c.805G > A p.G269S adult-onset TSD mutation. This putative adult-onset TSD c.748G > A p.G250S mutation has a population frequency similar to the common 7.6 kb deletion mutation that occurs in persons of French Canadian ancestry. Conclusions: We estimate the frequency of deleterious TSD alleles in Franco-Americans to be 1:73 (95% confidence interval 1:55 to 1:107). These data provide a more complete data base from which to formulate policy recommendations regarding TSD heterozygosity screening in individuals of French Canadian background. © 2007 American Association for Clinical Chemistry.

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Martin, D. C., Mark, B. L., Triggs-Raine, B. L., & Natowicz, M. R. (2007). Evaluation of the risk for Tay-Sachs disease in individuals of French Canadian ancestry living in New England. Clinical Chemistry, 53(3), 392–398. https://doi.org/10.1373/clinchem.2006.082727

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