CONFIRMATION OF CHROMOSOME-9P LINKAGE IN FAMILIAL MELANOMA

被引:0
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作者
NANCARROW, DJ
MANN, GJ
HOLLAND, EA
WALKER, GJ
BEATON, SC
WALTERS, MK
LUXFORD, C
PALMER, JM
DONALD, JA
WEBER, JL
FOUNTAIN, JW
KEFFORD, RF
HAYWARD, NK
机构
[1] QUEENSLAND INST MED RES,JOINT EXPTL ONCOL PROGRAM,QUEENSLAND CANC FUND RES UNIT,HERSTON 4029,AUSTRALIA
[2] UNIV SYDNEY,WESTMEAD CTR,DEPT MED ONCOL,SYDNEY,NSW 2006,AUSTRALIA
[3] MACQUARIE UNIV,SCH BIOL SCI,N RYDE,NSW 2113,AUSTRALIA
[4] MARSHFIELD MED RES FDN,MARSHFIELD,WI
[5] MIT,DEPT BIOL,CTR CANC RES,CAMBRIDGE,MA 02139
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D O I
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中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Malignant melanoma occurs as a familial cancer in 5%-10% of cases where it segregates in a manner consistent with autosomal dominant inheritance. Evidence from cytogenetics, fine-mapping studies of deletions in melanomas, and recent linkage studies supports the location of a human melanoma predisposition gene on the short arm of chromosome 9. We have carried out linkage analysis using the 9p markers IFNA and D9S126 in 26 Australian melanoma kindreds. Multipoint analysis gave a peak lod score of 4.43, 15 cM centromeric to D9S126, although a lod score of 4.13 was also found 15 cM telomeric of IFNA. These data confirm the existence of a melanoma susceptibility gene on 9p and indicate that this locus most probably lies outside of the IFNA-D9S126 interval. No significant heterogeneity was found between families, when either pairwise or multipoint data were analyzed using HOMOG.
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页码:936 / 942
页数:7
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