No evidence for linkage of long QT syndrome and chromosome 11p15.5 markers in a Chinese family: evidence for genetic heterogeneity

Yu Lin Ko; Shih Ann Chen; Tang K. Tang; Jiunn Lee Lin; Chern En Chiang; Jin Jer Chen; Ming Sheng Teng; Mau Song Chang; Wen Pin Lien; Cheng Wen Wu

doi:10.1007/BF00201594

No evidence for linkage of long QT syndrome and chromosome 11p15.5 markers in a Chinese family: evidence for genetic heterogeneity

Yu Lin Ko^*
, Shih Ann Chen
, Tang K. Tang
, Jiunn Lee Lin
, Chern En Chiang
, Jin Jer Chen
, Ming Sheng Teng
, Mau Song Chang
, Wen Pin Lien
, Cheng Wen Wu

^*此作品的通信作者

Academia Sinica - Institute of Biomedical Sciences
National Taiwan University
Veterans General Hospital-Taipei

研究成果: 期刊稿件 › 文章 › 同行評審

3 引文斯高帕斯（Scopus）

摘要

Recently the defective gene locus in seven Caucasian families with the Romano-Ward form of long QT syndrome (LQT) has been mapped to chromosome 11p. To understand the molecular basis of LQT in Chinese, a three-generation family was investigated. Fourteen family members were studied and five individuals were diagnosed to be affected, according to electrocardiographic criteria. Two genomic DNA probes (c-Ha-ras-3′-HVR and insulin-5′-HVR) and one tetranucleotide repeat polymorphism (THZ) derived from chromosome 11p15.5 loci and previously demonstrated to be closely linked to LQT were used as probes to analyze this family. A lod score of less than -2 was noted for all three polymorphisms. Our data show that there was no evidence of linkage between these three loci and the gene for LQT in this studied family. We believe that this result provides additional evidence for genetic heterogeneity of LQT.

原文	英語
頁（從 - 到）	364-366
頁數	3
期刊	Human Genetics
卷	94
發行號	4
DOIs	https://doi.org/10.1007/BF00201594
出版狀態	已出版 - 10 1994
對外發佈	是

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title = "No evidence for linkage of long QT syndrome and chromosome 11p15.5 markers in a Chinese family: evidence for genetic heterogeneity",

abstract = "Recently the defective gene locus in seven Caucasian families with the Romano-Ward form of long QT syndrome (LQT) has been mapped to chromosome 11p. To understand the molecular basis of LQT in Chinese, a three-generation family was investigated. Fourteen family members were studied and five individuals were diagnosed to be affected, according to electrocardiographic criteria. Two genomic DNA probes (c-Ha-ras-3′-HVR and insulin-5′-HVR) and one tetranucleotide repeat polymorphism (THZ) derived from chromosome 11p15.5 loci and previously demonstrated to be closely linked to LQT were used as probes to analyze this family. A lod score of less than -2 was noted for all three polymorphisms. Our data show that there was no evidence of linkage between these three loci and the gene for LQT in this studied family. We believe that this result provides additional evidence for genetic heterogeneity of LQT.",

author = "Ko, \{Yu Lin\} and Chen, \{Shih Ann\} and Tang, \{Tang K.\} and Lin, \{Jiunn Lee\} and Chiang, \{Chern En\} and Chen, \{Jin Jer\} and Teng, \{Ming Sheng\} and Chang, \{Mau Song\} and Lien, \{Wen Pin\} and Wu, \{Cheng Wen\}",

year = "1994",

month = oct,

doi = "10.1007/BF00201594",

language = "英语",

volume = "94",

pages = "364--366",

journal = "Human Genetics",

issn = "0340-6717",

publisher = "Springer Science and Business Media Deutschland GmbH",

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}

TY - JOUR

T1 - No evidence for linkage of long QT syndrome and chromosome 11p15.5 markers in a Chinese family

T2 - evidence for genetic heterogeneity

AU - Ko, Yu Lin

AU - Chen, Shih Ann

AU - Tang, Tang K.

AU - Lin, Jiunn Lee

AU - Chiang, Chern En

AU - Chen, Jin Jer

AU - Teng, Ming Sheng

AU - Chang, Mau Song

AU - Lien, Wen Pin

AU - Wu, Cheng Wen

PY - 1994/10

Y1 - 1994/10

N2 - Recently the defective gene locus in seven Caucasian families with the Romano-Ward form of long QT syndrome (LQT) has been mapped to chromosome 11p. To understand the molecular basis of LQT in Chinese, a three-generation family was investigated. Fourteen family members were studied and five individuals were diagnosed to be affected, according to electrocardiographic criteria. Two genomic DNA probes (c-Ha-ras-3′-HVR and insulin-5′-HVR) and one tetranucleotide repeat polymorphism (THZ) derived from chromosome 11p15.5 loci and previously demonstrated to be closely linked to LQT were used as probes to analyze this family. A lod score of less than -2 was noted for all three polymorphisms. Our data show that there was no evidence of linkage between these three loci and the gene for LQT in this studied family. We believe that this result provides additional evidence for genetic heterogeneity of LQT.

AB - Recently the defective gene locus in seven Caucasian families with the Romano-Ward form of long QT syndrome (LQT) has been mapped to chromosome 11p. To understand the molecular basis of LQT in Chinese, a three-generation family was investigated. Fourteen family members were studied and five individuals were diagnosed to be affected, according to electrocardiographic criteria. Two genomic DNA probes (c-Ha-ras-3′-HVR and insulin-5′-HVR) and one tetranucleotide repeat polymorphism (THZ) derived from chromosome 11p15.5 loci and previously demonstrated to be closely linked to LQT were used as probes to analyze this family. A lod score of less than -2 was noted for all three polymorphisms. Our data show that there was no evidence of linkage between these three loci and the gene for LQT in this studied family. We believe that this result provides additional evidence for genetic heterogeneity of LQT.

UR - https://www.scopus.com/pages/publications/0027981106

U2 - 10.1007/BF00201594

DO - 10.1007/BF00201594

M3 - 文章

C2 - 7927330

AN - SCOPUS:0027981106

SN - 0340-6717

VL - 94

SP - 364

EP - 366

JO - Human Genetics

JF - Human Genetics

IS - 4

ER -

No evidence for linkage of long QT syndrome and chromosome 11p15.5 markers in a Chinese family: evidence for genetic heterogeneity

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