Genetic analysis of familial myelodysplastic syndrome: Absence of linkage to chromosomes 5q31 and 7q22

Susan G. Mandla; Sharan Goobie; R. Tinny Kumar; Ormille Hayne; Ekram Zayed; Duane L. Guernsey; Wenda L. Greer

doi:10.1016/S0165-4608(98)00017-X

Genetic analysis of familial myelodysplastic syndrome: Absence of linkage to chromosomes 5q31 and 7q22

Susan G. Mandla, Sharan Goobie, R. Tinny Kumar, Ormille Hayne, Ekram Zayed, Duane L. Guernsey, Wenda L. Greer

Medicine

Medicine

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16 Citas (Scopus)

Resumen

Myelodysplastic syndrome (MDS) is a hematological disorder that occurs primarily in the elderly as an acquired, sporadic disease. Familial cases of MDS are rare. We have identified a kindred with three affected individuals, with early age of onset, suggesting a possible inherited predisposition to this disease. Using a molecular genetic approach, we examined whether bands 5q31 or 7q22 or both, the chromosomal regions most frequently associated with sporadic MDS, are involved in familial expression of MDS in this pedigree. Linkage analysis using polymorphic microsatellite DNA markers demonstrated that neither 5q31 nor 7q22 cosegregated with MDS in this family. There was no history of common environmental or occupational exposure among family members with MDS. In addition, analysis of polymorphisms at two loci [glutathione S- transferase T1 and M1 (GSTT1 and GSTM1)] involved in carcinogen detoxification and associated with cancer susceptibility, including increased risk for MDS, showed no evidence for enhanced sensitivity to environmental carcinogens in affected family members. Taken together, our findings suggest that (1) there is an inherited predisposition to MDS in this kindred; and (2) genes at 5q31 and 7q22, the regions most commonly associated with sporadic MDS, are excluded from a causal role in this family's disease.

Idioma original	English
Páginas (desde-hasta)	113-118
Número de páginas	6
Publicación	Cancer Genetics and Cytogenetics
Volumen	105
N.º	2
DOI	https://doi.org/10.1016/S0165-4608(98)00017-X
Estado	Published - sep. 1998

Nota bibliográfica

Funding Information:
We gratefully acknowledge the cooperation of all family members and their physicians. We thank Christine Lee for cytogenetic data; Annette Foyle for autopsy material; Vicki Stergiopoulos for preliminary data; Lynne Gallant for technical advice; and our colleagues from the Division of Molecular Pathology and Molecular Genetics for helpful discussion. This study was funded by a grant form Dalhousie University Faculty of Medicine and The Cancer Research Society Inc. of Montreal. S. G. M. is the recipient of an Oncology Fellowship Award form the Nova Scotia Division of the Canadian Cancer Society.

ASJC Scopus Subject Areas

Molecular Biology
Genetics
Cancer Research

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@article{ce83fc422b4442a4ac27eb4525036016,

title = "Genetic analysis of familial myelodysplastic syndrome: Absence of linkage to chromosomes 5q31 and 7q22",

abstract = "Myelodysplastic syndrome (MDS) is a hematological disorder that occurs primarily in the elderly as an acquired, sporadic disease. Familial cases of MDS are rare. We have identified a kindred with three affected individuals, with early age of onset, suggesting a possible inherited predisposition to this disease. Using a molecular genetic approach, we examined whether bands 5q31 or 7q22 or both, the chromosomal regions most frequently associated with sporadic MDS, are involved in familial expression of MDS in this pedigree. Linkage analysis using polymorphic microsatellite DNA markers demonstrated that neither 5q31 nor 7q22 cosegregated with MDS in this family. There was no history of common environmental or occupational exposure among family members with MDS. In addition, analysis of polymorphisms at two loci [glutathione S- transferase T1 and M1 (GSTT1 and GSTM1)] involved in carcinogen detoxification and associated with cancer susceptibility, including increased risk for MDS, showed no evidence for enhanced sensitivity to environmental carcinogens in affected family members. Taken together, our findings suggest that (1) there is an inherited predisposition to MDS in this kindred; and (2) genes at 5q31 and 7q22, the regions most commonly associated with sporadic MDS, are excluded from a causal role in this family's disease.",

author = "Mandla, {Susan G.} and Sharan Goobie and Kumar, {R. Tinny} and Ormille Hayne and Ekram Zayed and Guernsey, {Duane L.} and Greer, {Wenda L.}",

note = "Funding Information: We gratefully acknowledge the cooperation of all family members and their physicians. We thank Christine Lee for cytogenetic data; Annette Foyle for autopsy material; Vicki Stergiopoulos for preliminary data; Lynne Gallant for technical advice; and our colleagues from the Division of Molecular Pathology and Molecular Genetics for helpful discussion. This study was funded by a grant form Dalhousie University Faculty of Medicine and The Cancer Research Society Inc. of Montreal. S. G. M. is the recipient of an Oncology Fellowship Award form the Nova Scotia Division of the Canadian Cancer Society. ",

year = "1998",

month = sep,

doi = "10.1016/S0165-4608(98)00017-X",

language = "English",

volume = "105",

pages = "113--118",

journal = "Cancer Genetics and Cytogenetics",

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T2 - Absence of linkage to chromosomes 5q31 and 7q22

AU - Mandla, Susan G.

AU - Goobie, Sharan

AU - Kumar, R. Tinny

AU - Hayne, Ormille

AU - Zayed, Ekram

AU - Guernsey, Duane L.

AU - Greer, Wenda L.

N1 - Funding Information: We gratefully acknowledge the cooperation of all family members and their physicians. We thank Christine Lee for cytogenetic data; Annette Foyle for autopsy material; Vicki Stergiopoulos for preliminary data; Lynne Gallant for technical advice; and our colleagues from the Division of Molecular Pathology and Molecular Genetics for helpful discussion. This study was funded by a grant form Dalhousie University Faculty of Medicine and The Cancer Research Society Inc. of Montreal. S. G. M. is the recipient of an Oncology Fellowship Award form the Nova Scotia Division of the Canadian Cancer Society.

PY - 1998/9

Y1 - 1998/9

N2 - Myelodysplastic syndrome (MDS) is a hematological disorder that occurs primarily in the elderly as an acquired, sporadic disease. Familial cases of MDS are rare. We have identified a kindred with three affected individuals, with early age of onset, suggesting a possible inherited predisposition to this disease. Using a molecular genetic approach, we examined whether bands 5q31 or 7q22 or both, the chromosomal regions most frequently associated with sporadic MDS, are involved in familial expression of MDS in this pedigree. Linkage analysis using polymorphic microsatellite DNA markers demonstrated that neither 5q31 nor 7q22 cosegregated with MDS in this family. There was no history of common environmental or occupational exposure among family members with MDS. In addition, analysis of polymorphisms at two loci [glutathione S- transferase T1 and M1 (GSTT1 and GSTM1)] involved in carcinogen detoxification and associated with cancer susceptibility, including increased risk for MDS, showed no evidence for enhanced sensitivity to environmental carcinogens in affected family members. Taken together, our findings suggest that (1) there is an inherited predisposition to MDS in this kindred; and (2) genes at 5q31 and 7q22, the regions most commonly associated with sporadic MDS, are excluded from a causal role in this family's disease.

AB - Myelodysplastic syndrome (MDS) is a hematological disorder that occurs primarily in the elderly as an acquired, sporadic disease. Familial cases of MDS are rare. We have identified a kindred with three affected individuals, with early age of onset, suggesting a possible inherited predisposition to this disease. Using a molecular genetic approach, we examined whether bands 5q31 or 7q22 or both, the chromosomal regions most frequently associated with sporadic MDS, are involved in familial expression of MDS in this pedigree. Linkage analysis using polymorphic microsatellite DNA markers demonstrated that neither 5q31 nor 7q22 cosegregated with MDS in this family. There was no history of common environmental or occupational exposure among family members with MDS. In addition, analysis of polymorphisms at two loci [glutathione S- transferase T1 and M1 (GSTT1 and GSTM1)] involved in carcinogen detoxification and associated with cancer susceptibility, including increased risk for MDS, showed no evidence for enhanced sensitivity to environmental carcinogens in affected family members. Taken together, our findings suggest that (1) there is an inherited predisposition to MDS in this kindred; and (2) genes at 5q31 and 7q22, the regions most commonly associated with sporadic MDS, are excluded from a causal role in this family's disease.

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JO - Cancer Genetics and Cytogenetics

JF - Cancer Genetics and Cytogenetics

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ER -

Genetic analysis of familial myelodysplastic syndrome: Absence of linkage to chromosomes 5q31 and 7q22

Resumen

Nota bibliográfica

ASJC Scopus Subject Areas

ODS de las Naciones Unidas

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