The molecular basis of focal cyst formation in human autosomal dominant polycystic kidney disease type I

Feng Qian; Terry J. Watnick; Luiz F. Onuchic; Gregory G. Germino

doi:10.1016/S0092-8674(00)81793-6

The molecular basis of focal cyst formation in human autosomal dominant polycystic kidney disease type I

Feng Qian, Terry J. Watnick, Luiz F. Onuchic, Gregory G. Germino

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

457 Scopus citations

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is a common disease and an important cause of renal failure. It is characterized by considerable intrafamilial phenotypic variation and focal cyst formation. To elucidate the molecular basis for these observations, we have developed a novel method for isolating renal cystic epithelia from single cysts and have used it to show that individual renal cysts in ADPKD are monoclonal. Loss of heterozygosity was discovered within a subset of cysts for two closely linked polymorphic markers located within the PKD1 gene. Genetic analysis revealed that it was the normal haplotype that was lost. This study provides a molecular explanation for the focal nature of cyst formation and a probable mechanism whereby mutations cause disease. The high rate at which 'second hits' must occur to account for the large number of cysts observed suggests that unique structural features of the PKD1 gene may be responsible for its mutability.

Original language	English (US)
Pages (from-to)	979-987
Number of pages	9
Journal	Cell
Volume	87
Issue number	6
DOIs	https://doi.org/10.1016/S0092-8674(00)81793-6
State	Published - Dec 13 1996
Externally published	Yes

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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title = "The molecular basis of focal cyst formation in human autosomal dominant polycystic kidney disease type I",

abstract = "Autosomal dominant polycystic kidney disease (ADPKD) is a common disease and an important cause of renal failure. It is characterized by considerable intrafamilial phenotypic variation and focal cyst formation. To elucidate the molecular basis for these observations, we have developed a novel method for isolating renal cystic epithelia from single cysts and have used it to show that individual renal cysts in ADPKD are monoclonal. Loss of heterozygosity was discovered within a subset of cysts for two closely linked polymorphic markers located within the PKD1 gene. Genetic analysis revealed that it was the normal haplotype that was lost. This study provides a molecular explanation for the focal nature of cyst formation and a probable mechanism whereby mutations cause disease. The high rate at which 'second hits' must occur to account for the large number of cysts observed suggests that unique structural features of the PKD1 gene may be responsible for its mutability.",

author = "Feng Qian and Watnick, {Terry J.} and Onuchic, {Luiz F.} and Germino, {Gregory G.}",

note = "Funding Information: Correspondence should be addressed to G. G. G. We are grateful to all ADPKD family members for their invaluable participation and the Polycystic Kidney Research Foundation for assistance in the collection of tissue samples used in the study. We thank Xiangbin Zhang, Edward Lee, and Martin Daoust for their help in cyst preparation; Dr. Klaus Piontek and Sidney McGaughey for their help in the preparation of the manuscript; Dr. Irene Maumenee and Thomas Mitchell of the Johns Hopkins Hereditary Eye Center for assistance in the linkage calculations; and Dr. Joseph Handler for helpful discussions. This work was supported by the Polycystic Kidney Research Foundation (grant 95004), the National Insitutes of Health (grant DK48006), and the McKutcheon Foundation. G. G. G. is the Irving Blum Scholar of The Johns Hopkins University School of Medicine. ",

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N1 - Funding Information: Correspondence should be addressed to G. G. G. We are grateful to all ADPKD family members for their invaluable participation and the Polycystic Kidney Research Foundation for assistance in the collection of tissue samples used in the study. We thank Xiangbin Zhang, Edward Lee, and Martin Daoust for their help in cyst preparation; Dr. Klaus Piontek and Sidney McGaughey for their help in the preparation of the manuscript; Dr. Irene Maumenee and Thomas Mitchell of the Johns Hopkins Hereditary Eye Center for assistance in the linkage calculations; and Dr. Joseph Handler for helpful discussions. This work was supported by the Polycystic Kidney Research Foundation (grant 95004), the National Insitutes of Health (grant DK48006), and the McKutcheon Foundation. G. G. G. is the Irving Blum Scholar of The Johns Hopkins University School of Medicine.

PY - 1996/12/13

Y1 - 1996/12/13

N2 - Autosomal dominant polycystic kidney disease (ADPKD) is a common disease and an important cause of renal failure. It is characterized by considerable intrafamilial phenotypic variation and focal cyst formation. To elucidate the molecular basis for these observations, we have developed a novel method for isolating renal cystic epithelia from single cysts and have used it to show that individual renal cysts in ADPKD are monoclonal. Loss of heterozygosity was discovered within a subset of cysts for two closely linked polymorphic markers located within the PKD1 gene. Genetic analysis revealed that it was the normal haplotype that was lost. This study provides a molecular explanation for the focal nature of cyst formation and a probable mechanism whereby mutations cause disease. The high rate at which 'second hits' must occur to account for the large number of cysts observed suggests that unique structural features of the PKD1 gene may be responsible for its mutability.

AB - Autosomal dominant polycystic kidney disease (ADPKD) is a common disease and an important cause of renal failure. It is characterized by considerable intrafamilial phenotypic variation and focal cyst formation. To elucidate the molecular basis for these observations, we have developed a novel method for isolating renal cystic epithelia from single cysts and have used it to show that individual renal cysts in ADPKD are monoclonal. Loss of heterozygosity was discovered within a subset of cysts for two closely linked polymorphic markers located within the PKD1 gene. Genetic analysis revealed that it was the normal haplotype that was lost. This study provides a molecular explanation for the focal nature of cyst formation and a probable mechanism whereby mutations cause disease. The high rate at which 'second hits' must occur to account for the large number of cysts observed suggests that unique structural features of the PKD1 gene may be responsible for its mutability.

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The molecular basis of focal cyst formation in human autosomal dominant polycystic kidney disease type I

Abstract

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