Linkage homogeneity near the fragile X locus in normal and fragile X families

G. K. Suthers; J. C. Mulley; M. A. Voelckel; N. Dahl; M. L. Väisänen; P. Steinbach; I. A. Glass; C. E. Schwartz; B. A. van Oost; S. N. Thibodeau; N. E. Haites; B. A. Oostra; A. Schinzel; M. Carballo; C. P. Morris; J. J. Hopwood; G. R. Sutherland

doi:10.1016/0888-7543(91)90438-K

Linkage homogeneity near the fragile X locus in normal and fragile X families

G. K. Suthers, J. C. Mulley, M. A. Voelckel, N. Dahl, M. L. Väisänen, P. Steinbach, I. A. Glass, C. E. Schwartz, B. A. van Oost, S. N. Thibodeau, N. E. Haites, B. A. Oostra, A. Schinzel, M. Carballo, C. P. Morris, J. J. Hopwood, G. R. Sutherland

Laboratory Medicine and Pathology

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

7 Scopus citations

Abstract

The fragile X syndrome locus, FRAXA, is located at Xq27. Until recently, few polymorphic loci had been genetically mapped close to FRAXA. This has been attributed to an increased frequency of recombination at Xq27, possibly associated with the fragile X mutation. In addition, the frequency of recombination around FRAXA has been reported to vary among fragile X families. These observations suggested that the genetic map at Xq27 in normal populations was different from that in fragile X populations and that the genetic map also varied within the fragile X population. Such variability would reduce the reliability of carrier risk estimates based on DNA studies in fragile X families. Five polymorphic loci have now been mapped to within 4 cM of FRAXA-DXS369, DXS297, DXS296, IDS, and DXS304. The frequency of recombination at Xq26-q28 was evaluated using data at these loci and at more distant loci from 112 families with the fragile X syndrome. Two-point and multipoint linkage analyses failed to detect any difference in the recombination fractions in fragile X versus normal families. Two-point and multipoint tests of linkage homogeneity neity failed to detect any evidence of linkage heterogeneity in the fragile X families. On the basis of this analysis, genetic maps derived from large samples of normal familes and those derived from fragile X families are equally valid as the basis for calculating carrier risk estimates in a particular family.

Original language	English (US)
Pages (from-to)	576-582
Number of pages	7
Journal	Genomics
Volume	10
Issue number	3
DOIs	https://doi.org/10.1016/0888-7543(91)90438-K
State	Published - Jul 1991

ASJC Scopus subject areas

Genetics

Access to Document

10.1016/0888-7543(91)90438-K

Cite this

Suthers, G. K., Mulley, J. C., Voelckel, M. A., Dahl, N., Väisänen, M. L., Steinbach, P., Glass, I. A., Schwartz, C. E., van Oost, B. A., Thibodeau, S. N., Haites, N. E., Oostra, B. A., Schinzel, A., Carballo, M., Morris, C. P., Hopwood, J. J., & Sutherland, G. R. (1991). Linkage homogeneity near the fragile X locus in normal and fragile X families. Genomics, 10(3), 576-582. https://doi.org/10.1016/0888-7543(91)90438-K

Suthers, GK, Mulley, JC, Voelckel, MA, Dahl, N, Väisänen, ML, Steinbach, P, Glass, IA, Schwartz, CE, van Oost, BA, Thibodeau, SN, Haites, NE, Oostra, BA, Schinzel, A, Carballo, M, Morris, CP, Hopwood, JJ & Sutherland, GR 1991, 'Linkage homogeneity near the fragile X locus in normal and fragile X families', Genomics, vol. 10, no. 3, pp. 576-582. https://doi.org/10.1016/0888-7543(91)90438-K

@article{c07747d2dacb4d0ebefe6be05408b259,

title = "Linkage homogeneity near the fragile X locus in normal and fragile X families",

abstract = "The fragile X syndrome locus, FRAXA, is located at Xq27. Until recently, few polymorphic loci had been genetically mapped close to FRAXA. This has been attributed to an increased frequency of recombination at Xq27, possibly associated with the fragile X mutation. In addition, the frequency of recombination around FRAXA has been reported to vary among fragile X families. These observations suggested that the genetic map at Xq27 in normal populations was different from that in fragile X populations and that the genetic map also varied within the fragile X population. Such variability would reduce the reliability of carrier risk estimates based on DNA studies in fragile X families. Five polymorphic loci have now been mapped to within 4 cM of FRAXA-DXS369, DXS297, DXS296, IDS, and DXS304. The frequency of recombination at Xq26-q28 was evaluated using data at these loci and at more distant loci from 112 families with the fragile X syndrome. Two-point and multipoint linkage analyses failed to detect any difference in the recombination fractions in fragile X versus normal families. Two-point and multipoint tests of linkage homogeneity neity failed to detect any evidence of linkage heterogeneity in the fragile X families. On the basis of this analysis, genetic maps derived from large samples of normal familes and those derived from fragile X families are equally valid as the basis for calculating carrier risk estimates in a particular family.",

author = "Suthers, {G. K.} and Mulley, {J. C.} and Voelckel, {M. A.} and N. Dahl and V{\"a}is{\"a}nen, {M. L.} and P. Steinbach and Glass, {I. A.} and Schwartz, {C. E.} and {van Oost}, {B. A.} and Thibodeau, {S. N.} and Haites, {N. E.} and Oostra, {B. A.} and A. Schinzel and M. Carballo and Morris, {C. P.} and Hopwood, {J. J.} and Sutherland, {G. R.}",

note = "Funding Information: We thank the many colleagues and forbearing families who made this study possible. We acknowledge the advice and assistance of M. C. Pellisier, I. Boccaccio, U. Pettersson, J. 0. Ulmer, A. Smits, J. C. F. M. Dreesen, and R. Gin& The LINKAGE and HO-MOG programs were provided by Dr. J. Ott of Columbia University. This project was supported by the National Health and Medical Research Council of Australia, the Adelaide Children{\textquoteright}s Hospital Research Foundation, CNAM and Association Francaise, the Swedish Medical Research Council, Sigrid Juselius Foundation, Deutsche Forschungsgemeinschaft DFG, Grampian Health Board, and Scottish Hospitals Endowments Research Trust. Copyright: Copyright 2014 Elsevier B.V., All rights reserved.",

year = "1991",

month = jul,

doi = "10.1016/0888-7543(91)90438-K",

language = "English (US)",

volume = "10",

pages = "576--582",

journal = "Genomics",

issn = "0888-7543",

publisher = "Academic Press Inc.",

number = "3",

}

TY - JOUR

T1 - Linkage homogeneity near the fragile X locus in normal and fragile X families

AU - Suthers, G. K.

AU - Mulley, J. C.

AU - Voelckel, M. A.

AU - Dahl, N.

AU - Väisänen, M. L.

AU - Steinbach, P.

AU - Glass, I. A.

AU - Schwartz, C. E.

AU - van Oost, B. A.

AU - Thibodeau, S. N.

AU - Haites, N. E.

AU - Oostra, B. A.

AU - Schinzel, A.

AU - Carballo, M.

AU - Morris, C. P.

AU - Hopwood, J. J.

AU - Sutherland, G. R.

N1 - Funding Information: We thank the many colleagues and forbearing families who made this study possible. We acknowledge the advice and assistance of M. C. Pellisier, I. Boccaccio, U. Pettersson, J. 0. Ulmer, A. Smits, J. C. F. M. Dreesen, and R. Gin& The LINKAGE and HO-MOG programs were provided by Dr. J. Ott of Columbia University. This project was supported by the National Health and Medical Research Council of Australia, the Adelaide Children’s Hospital Research Foundation, CNAM and Association Francaise, the Swedish Medical Research Council, Sigrid Juselius Foundation, Deutsche Forschungsgemeinschaft DFG, Grampian Health Board, and Scottish Hospitals Endowments Research Trust. Copyright: Copyright 2014 Elsevier B.V., All rights reserved.

PY - 1991/7

Y1 - 1991/7

N2 - The fragile X syndrome locus, FRAXA, is located at Xq27. Until recently, few polymorphic loci had been genetically mapped close to FRAXA. This has been attributed to an increased frequency of recombination at Xq27, possibly associated with the fragile X mutation. In addition, the frequency of recombination around FRAXA has been reported to vary among fragile X families. These observations suggested that the genetic map at Xq27 in normal populations was different from that in fragile X populations and that the genetic map also varied within the fragile X population. Such variability would reduce the reliability of carrier risk estimates based on DNA studies in fragile X families. Five polymorphic loci have now been mapped to within 4 cM of FRAXA-DXS369, DXS297, DXS296, IDS, and DXS304. The frequency of recombination at Xq26-q28 was evaluated using data at these loci and at more distant loci from 112 families with the fragile X syndrome. Two-point and multipoint linkage analyses failed to detect any difference in the recombination fractions in fragile X versus normal families. Two-point and multipoint tests of linkage homogeneity neity failed to detect any evidence of linkage heterogeneity in the fragile X families. On the basis of this analysis, genetic maps derived from large samples of normal familes and those derived from fragile X families are equally valid as the basis for calculating carrier risk estimates in a particular family.

AB - The fragile X syndrome locus, FRAXA, is located at Xq27. Until recently, few polymorphic loci had been genetically mapped close to FRAXA. This has been attributed to an increased frequency of recombination at Xq27, possibly associated with the fragile X mutation. In addition, the frequency of recombination around FRAXA has been reported to vary among fragile X families. These observations suggested that the genetic map at Xq27 in normal populations was different from that in fragile X populations and that the genetic map also varied within the fragile X population. Such variability would reduce the reliability of carrier risk estimates based on DNA studies in fragile X families. Five polymorphic loci have now been mapped to within 4 cM of FRAXA-DXS369, DXS297, DXS296, IDS, and DXS304. The frequency of recombination at Xq26-q28 was evaluated using data at these loci and at more distant loci from 112 families with the fragile X syndrome. Two-point and multipoint linkage analyses failed to detect any difference in the recombination fractions in fragile X versus normal families. Two-point and multipoint tests of linkage homogeneity neity failed to detect any evidence of linkage heterogeneity in the fragile X families. On the basis of this analysis, genetic maps derived from large samples of normal familes and those derived from fragile X families are equally valid as the basis for calculating carrier risk estimates in a particular family.

UR - http://www.scopus.com/inward/record.url?scp=0025836727&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=0025836727&partnerID=8YFLogxK

U2 - 10.1016/0888-7543(91)90438-K

DO - 10.1016/0888-7543(91)90438-K

M3 - Article

C2 - 1889808

AN - SCOPUS:0025836727

SN - 0888-7543

VL - 10

SP - 576

EP - 582

JO - Genomics

JF - Genomics

IS - 3

ER -

Linkage homogeneity near the fragile X locus in normal and fragile X families

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this