Unreliability of the microcomplement fixation method for Xga typing of cultured fibroblasts

S. H. Hsu; B. R. Migeon; W. B. Bias

doi:10.1159/000130638

Unreliability of the microcomplement fixation method for Xg^a typing of cultured fibroblasts

S. H. Hsu, B. R. Migeon, W. B. Bias

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2 Scopus citations

Abstract

Evidence pointing to localization of the Xg locus on either the long or short arm of the X chromosome is conflicting. Whether the Xg locus is subject to X inactivation is also undecided. A report that Xg antigen could be detected on cultured fibroblasts or in hybridized cell lines by microcomplement fixation seemed to open new possibilities of studying these important problems. Indeed, Fellous et al., using the microcomplement fixation method, mapped the Xg locus to the short arm of the X chromosome by typing a human cell line involving a translocation, t(X;17)(p11;q20), of the X and chromosome 17. However, the authors were unable to duplicate the results of Fellous et al., whether they used their technique or their own.

Original language	English (US)
Pages (from-to)	382-386
Number of pages	5
Journal	Cytogenetics and cell genetics
Volume	16
Issue number	1-5
DOIs	https://doi.org/10.1159/000130638
State	Published - 1976
Externally published	Yes

ASJC Scopus subject areas

Genetics
Cell Biology

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title = "Unreliability of the microcomplement fixation method for Xga typing of cultured fibroblasts",

abstract = "Evidence pointing to localization of the Xg locus on either the long or short arm of the X chromosome is conflicting. Whether the Xg locus is subject to X inactivation is also undecided. A report that Xg antigen could be detected on cultured fibroblasts or in hybridized cell lines by microcomplement fixation seemed to open new possibilities of studying these important problems. Indeed, Fellous et al., using the microcomplement fixation method, mapped the Xg locus to the short arm of the X chromosome by typing a human cell line involving a translocation, t(X;17)(p11;q20), of the X and chromosome 17. However, the authors were unable to duplicate the results of Fellous et al., whether they used their technique or their own.",

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year = "1976",

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T1 - Unreliability of the microcomplement fixation method for Xga typing of cultured fibroblasts

AU - Hsu, S. H.

AU - Migeon, B. R.

AU - Bias, W. B.

PY - 1976

Y1 - 1976

N2 - Evidence pointing to localization of the Xg locus on either the long or short arm of the X chromosome is conflicting. Whether the Xg locus is subject to X inactivation is also undecided. A report that Xg antigen could be detected on cultured fibroblasts or in hybridized cell lines by microcomplement fixation seemed to open new possibilities of studying these important problems. Indeed, Fellous et al., using the microcomplement fixation method, mapped the Xg locus to the short arm of the X chromosome by typing a human cell line involving a translocation, t(X;17)(p11;q20), of the X and chromosome 17. However, the authors were unable to duplicate the results of Fellous et al., whether they used their technique or their own.

AB - Evidence pointing to localization of the Xg locus on either the long or short arm of the X chromosome is conflicting. Whether the Xg locus is subject to X inactivation is also undecided. A report that Xg antigen could be detected on cultured fibroblasts or in hybridized cell lines by microcomplement fixation seemed to open new possibilities of studying these important problems. Indeed, Fellous et al., using the microcomplement fixation method, mapped the Xg locus to the short arm of the X chromosome by typing a human cell line involving a translocation, t(X;17)(p11;q20), of the X and chromosome 17. However, the authors were unable to duplicate the results of Fellous et al., whether they used their technique or their own.

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Unreliability of the microcomplement fixation method for Xg^a typing of cultured fibroblasts

Abstract

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