A pseudodeficiency allele common in non-Jewish Tay-Sachs carriers: Implications for carrier screening

B. L. Triggs-Raine; E. H. Mules; M. M. Kaback; J. S.T. Lim-Steele; C. E. Dowling; B. R. Akerman; M. R. Natowicz; E. E. Grebner; R. Navon; J. P. Welch; C. R. Greenberg; G. H. Thomas; R. A. Gravel

A pseudodeficiency allele common in non-Jewish Tay-Sachs carriers: Implications for carrier screening

B. L. Triggs-Raine, E. H. Mules, M. M. Kaback, J. S.T. Lim-Steele, C. E. Dowling, B. R. Akerman, M. R. Natowicz, E. E. Grebner, R. Navon, J. P. Welch, C. R. Greenberg, G. H. Thomas, R. A. Gravel

Research output: Contribution to journal › Article › peer-review

52 Scopus citations

Abstract

Deficiency of β-hexosaminidase A (Hex A) activity typically results in Tay-Sachs disease. However, healthy subjects found to be deficient in Hex A activity (i.e., pseudodeficient) by means of in vitro biochemical tests have been described. We analyzed the HEXA gene of one pseudodeficient subject and identified both a C₇₃₉-to-T substitution that changes Arg₂₄₇→Trp on one allele and a previously identified Tay-Sachs disease mutation on the second allele. Six additional pseudodeficient subjects were found to have the C₇₃₉-to-T mutation. This allele accounted for 32% (20/62) of non-Jewish enzyme-defined Tay-Sachs disease carriers but for none of 36 Jewish enzyme-defined carriers who did not have one of three known mutations common to this group. The C₇₃₉-to-T allele, together with a "true" Tay-Sachs disease allele, causes Hex A pseudodeficiency. Given both the large proportion of non-Jewish carriers with this allele and that standard biochemical screening cannot differentiate between heterozygotes for the C₇₃₉-to-T mutations and Tay-Sachs disease carriers, DNA testing for this mutation in at-risk couples is essential. This could prevent unnecessary or incorrect prenatal diagnoses.

Original language	English (US)
Pages (from-to)	793-801
Number of pages	9
Journal	American journal of human genetics
Volume	51
Issue number	4
State	Published - Oct 1992
Externally published	Yes

ASJC Scopus subject areas

Genetics
Genetics(clinical)

Cite this

Triggs-Raine, B. L., Mules, E. H., Kaback, M. M., Lim-Steele, J. S. T., Dowling, C. E., Akerman, B. R., Natowicz, M. R., Grebner, E. E., Navon, R., Welch, J. P., Greenberg, C. R., Thomas, G. H., & Gravel, R. A. (1992). A pseudodeficiency allele common in non-Jewish Tay-Sachs carriers: Implications for carrier screening. American journal of human genetics, 51(4), 793-801.

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title = "A pseudodeficiency allele common in non-Jewish Tay-Sachs carriers: Implications for carrier screening",

abstract = "Deficiency of β-hexosaminidase A (Hex A) activity typically results in Tay-Sachs disease. However, healthy subjects found to be deficient in Hex A activity (i.e., pseudodeficient) by means of in vitro biochemical tests have been described. We analyzed the HEXA gene of one pseudodeficient subject and identified both a C739-to-T substitution that changes Arg247→Trp on one allele and a previously identified Tay-Sachs disease mutation on the second allele. Six additional pseudodeficient subjects were found to have the C739-to-T mutation. This allele accounted for 32% (20/62) of non-Jewish enzyme-defined Tay-Sachs disease carriers but for none of 36 Jewish enzyme-defined carriers who did not have one of three known mutations common to this group. The C739-to-T allele, together with a {"}true{"} Tay-Sachs disease allele, causes Hex A pseudodeficiency. Given both the large proportion of non-Jewish carriers with this allele and that standard biochemical screening cannot differentiate between heterozygotes for the C739-to-T mutations and Tay-Sachs disease carriers, DNA testing for this mutation in at-risk couples is essential. This could prevent unnecessary or incorrect prenatal diagnoses.",

author = "Triggs-Raine, {B. L.} and Mules, {E. H.} and Kaback, {M. M.} and Lim-Steele, {J. S.T.} and Dowling, {C. E.} and Akerman, {B. R.} and Natowicz, {M. R.} and Grebner, {E. E.} and R. Navon and Welch, {J. P.} and Greenberg, {C. R.} and Thomas, {G. H.} and Gravel, {R. A.}",

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T2 - Implications for carrier screening

AU - Triggs-Raine, B. L.

AU - Mules, E. H.

AU - Kaback, M. M.

AU - Lim-Steele, J. S.T.

AU - Dowling, C. E.

AU - Akerman, B. R.

AU - Natowicz, M. R.

AU - Grebner, E. E.

AU - Navon, R.

AU - Welch, J. P.

AU - Greenberg, C. R.

AU - Thomas, G. H.

AU - Gravel, R. A.

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N2 - Deficiency of β-hexosaminidase A (Hex A) activity typically results in Tay-Sachs disease. However, healthy subjects found to be deficient in Hex A activity (i.e., pseudodeficient) by means of in vitro biochemical tests have been described. We analyzed the HEXA gene of one pseudodeficient subject and identified both a C739-to-T substitution that changes Arg247→Trp on one allele and a previously identified Tay-Sachs disease mutation on the second allele. Six additional pseudodeficient subjects were found to have the C739-to-T mutation. This allele accounted for 32% (20/62) of non-Jewish enzyme-defined Tay-Sachs disease carriers but for none of 36 Jewish enzyme-defined carriers who did not have one of three known mutations common to this group. The C739-to-T allele, together with a "true" Tay-Sachs disease allele, causes Hex A pseudodeficiency. Given both the large proportion of non-Jewish carriers with this allele and that standard biochemical screening cannot differentiate between heterozygotes for the C739-to-T mutations and Tay-Sachs disease carriers, DNA testing for this mutation in at-risk couples is essential. This could prevent unnecessary or incorrect prenatal diagnoses.

AB - Deficiency of β-hexosaminidase A (Hex A) activity typically results in Tay-Sachs disease. However, healthy subjects found to be deficient in Hex A activity (i.e., pseudodeficient) by means of in vitro biochemical tests have been described. We analyzed the HEXA gene of one pseudodeficient subject and identified both a C739-to-T substitution that changes Arg247→Trp on one allele and a previously identified Tay-Sachs disease mutation on the second allele. Six additional pseudodeficient subjects were found to have the C739-to-T mutation. This allele accounted for 32% (20/62) of non-Jewish enzyme-defined Tay-Sachs disease carriers but for none of 36 Jewish enzyme-defined carriers who did not have one of three known mutations common to this group. The C739-to-T allele, together with a "true" Tay-Sachs disease allele, causes Hex A pseudodeficiency. Given both the large proportion of non-Jewish carriers with this allele and that standard biochemical screening cannot differentiate between heterozygotes for the C739-to-T mutations and Tay-Sachs disease carriers, DNA testing for this mutation in at-risk couples is essential. This could prevent unnecessary or incorrect prenatal diagnoses.

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A pseudodeficiency allele common in non-Jewish Tay-Sachs carriers: Implications for carrier screening

Abstract

ASJC Scopus subject areas

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