Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)

M. H. Breuning; F. G M Snijdewint; H. Brunner; A. Verwest; J. W. Ijdo; J. J. Saris; J. G. Dauwerse; L. Blonden; T. Keith; D. F. Callen; V. J. Hyland; G. H. Xiao; G. Scherer; D. R. Higgs; P. Harris; L. Bachner; S. T. Reeders; G. Germino; P. L. Pearson; G. J B Van Ommen

Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)

M. H. Breuning, F. G M Snijdewint, H. Brunner, A. Verwest, J. W. Ijdo, J. J. Saris, J. G. Dauwerse, L. Blonden, T. Keith, D. F. Callen, V. J. Hyland, G. H. Xiao, G. Scherer, D. R. Higgs, P. Harris, L. Bachner, S. T. Reeders, G. Germino, P. L. Pearson, G. J B Van Ommen

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

34 Scopus citations

Abstract

To define the PKD1 locus further, the gene involved in the most frequent form of adult polycystic kidney disease, probes from 16 polymorphic loci were mapped on 16p13.1-pter with the combined use of cell lines containing rearranged chromosomes and family studies. Five breakpoints in the distal part of 16p arbitrarily subdivided the loci into five groups. By analysing 58 recombination events among 259 informative meioses in 12 large families with PKD, we were able to construct a linkage map for the distal part of 16p. The order of the markers obtained with chromosomal rearrangements was confirmed by the family studies. The D16S85 locus near α globin, D16S21, and D16S83 map distal, or telomeric, to PKD1. The polymorphic red cell enzyme phosphoglycolate phosphatase (PGP), D16S84, D16S259, and D16S246 showed no recombination with PKD1. The remaining nine RFLPs all map proximal to the PKD1 gene. By cosmid walking, additional RFLPs were detected at the D16S21 locus. A single intrahaplotype recombination observed defines the orientation of D16S21 relative to PKD1. The new polymorphisms are valuable for presymptomatic and prenatal diagnosis of PKD1. Furthermore, our map is both a good starting point for the physical map of 16p and a useful tool for the isolation of the PKD1 gene.

Original language	English (US)
Pages (from-to)	603-613
Number of pages	11
Journal	Journal of Medical Genetics
Volume	27
Issue number	10
State	Published - Oct 1990
Externally published	Yes

ASJC Scopus subject areas

Genetics
Genetics(clinical)

Cite this

Breuning, M. H., Snijdewint, F. G. M., Brunner, H., Verwest, A., Ijdo, J. W., Saris, J. J., Dauwerse, J. G., Blonden, L., Keith, T., Callen, D. F., Hyland, V. J., Xiao, G. H., Scherer, G., Higgs, D. R., Harris, P., Bachner, L., Reeders, S. T., Germino, G., Pearson, P. L., & Van Ommen, G. J. B. (1990). Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1). Journal of Medical Genetics, 27(10), 603-613.

Breuning, MH, Snijdewint, FGM, Brunner, H, Verwest, A, Ijdo, JW, Saris, JJ, Dauwerse, JG, Blonden, L, Keith, T, Callen, DF, Hyland, VJ, Xiao, GH, Scherer, G, Higgs, DR, Harris, P, Bachner, L, Reeders, ST, Germino, G, Pearson, PL & Van Ommen, GJB 1990, 'Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)', Journal of Medical Genetics, vol. 27, no. 10, pp. 603-613.

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title = "Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)",

abstract = "To define the PKD1 locus further, the gene involved in the most frequent form of adult polycystic kidney disease, probes from 16 polymorphic loci were mapped on 16p13.1-pter with the combined use of cell lines containing rearranged chromosomes and family studies. Five breakpoints in the distal part of 16p arbitrarily subdivided the loci into five groups. By analysing 58 recombination events among 259 informative meioses in 12 large families with PKD, we were able to construct a linkage map for the distal part of 16p. The order of the markers obtained with chromosomal rearrangements was confirmed by the family studies. The D16S85 locus near α globin, D16S21, and D16S83 map distal, or telomeric, to PKD1. The polymorphic red cell enzyme phosphoglycolate phosphatase (PGP), D16S84, D16S259, and D16S246 showed no recombination with PKD1. The remaining nine RFLPs all map proximal to the PKD1 gene. By cosmid walking, additional RFLPs were detected at the D16S21 locus. A single intrahaplotype recombination observed defines the orientation of D16S21 relative to PKD1. The new polymorphisms are valuable for presymptomatic and prenatal diagnosis of PKD1. Furthermore, our map is both a good starting point for the physical map of 16p and a useful tool for the isolation of the PKD1 gene.",

author = "Breuning, {M. H.} and Snijdewint, {F. G M} and H. Brunner and A. Verwest and Ijdo, {J. W.} and Saris, {J. J.} and Dauwerse, {J. G.} and L. Blonden and T. Keith and Callen, {D. F.} and Hyland, {V. J.} and Xiao, {G. H.} and G. Scherer and Higgs, {D. R.} and P. Harris and L. Bachner and Reeders, {S. T.} and G. Germino and Pearson, {P. L.} and {Van Ommen}, {G. J B}",

year = "1990",

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language = "English (US)",

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T1 - Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)

AU - Breuning, M. H.

AU - Snijdewint, F. G M

AU - Brunner, H.

AU - Verwest, A.

AU - Ijdo, J. W.

AU - Saris, J. J.

AU - Dauwerse, J. G.

AU - Blonden, L.

AU - Keith, T.

AU - Callen, D. F.

AU - Hyland, V. J.

AU - Xiao, G. H.

AU - Scherer, G.

AU - Higgs, D. R.

AU - Harris, P.

AU - Bachner, L.

AU - Reeders, S. T.

AU - Germino, G.

AU - Pearson, P. L.

AU - Van Ommen, G. J B

PY - 1990/10

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N2 - To define the PKD1 locus further, the gene involved in the most frequent form of adult polycystic kidney disease, probes from 16 polymorphic loci were mapped on 16p13.1-pter with the combined use of cell lines containing rearranged chromosomes and family studies. Five breakpoints in the distal part of 16p arbitrarily subdivided the loci into five groups. By analysing 58 recombination events among 259 informative meioses in 12 large families with PKD, we were able to construct a linkage map for the distal part of 16p. The order of the markers obtained with chromosomal rearrangements was confirmed by the family studies. The D16S85 locus near α globin, D16S21, and D16S83 map distal, or telomeric, to PKD1. The polymorphic red cell enzyme phosphoglycolate phosphatase (PGP), D16S84, D16S259, and D16S246 showed no recombination with PKD1. The remaining nine RFLPs all map proximal to the PKD1 gene. By cosmid walking, additional RFLPs were detected at the D16S21 locus. A single intrahaplotype recombination observed defines the orientation of D16S21 relative to PKD1. The new polymorphisms are valuable for presymptomatic and prenatal diagnosis of PKD1. Furthermore, our map is both a good starting point for the physical map of 16p and a useful tool for the isolation of the PKD1 gene.

AB - To define the PKD1 locus further, the gene involved in the most frequent form of adult polycystic kidney disease, probes from 16 polymorphic loci were mapped on 16p13.1-pter with the combined use of cell lines containing rearranged chromosomes and family studies. Five breakpoints in the distal part of 16p arbitrarily subdivided the loci into five groups. By analysing 58 recombination events among 259 informative meioses in 12 large families with PKD, we were able to construct a linkage map for the distal part of 16p. The order of the markers obtained with chromosomal rearrangements was confirmed by the family studies. The D16S85 locus near α globin, D16S21, and D16S83 map distal, or telomeric, to PKD1. The polymorphic red cell enzyme phosphoglycolate phosphatase (PGP), D16S84, D16S259, and D16S246 showed no recombination with PKD1. The remaining nine RFLPs all map proximal to the PKD1 gene. By cosmid walking, additional RFLPs were detected at the D16S21 locus. A single intrahaplotype recombination observed defines the orientation of D16S21 relative to PKD1. The new polymorphisms are valuable for presymptomatic and prenatal diagnosis of PKD1. Furthermore, our map is both a good starting point for the physical map of 16p and a useful tool for the isolation of the PKD1 gene.

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ER -

Map of 16 polymorphic loci on the short arm of chromosome 16 close to the polycystic kidney disease gene (PKD1)

Abstract

ASJC Scopus subject areas

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