IDENTIFYING CHROMOSOMAL FRAGILE SITES FROM INDIVIDUALS - A MULTINOMIAL STATISTICAL-MODEL

被引:0
|
作者
BOHM, U
DAHM, PF
MCALLISTER, BF
GREENBAUM, IF
机构
[1] TEXAS A&M UNIV,DEPT STAT,COLLEGE STN,TX 77843
[2] TEXAS A&M UNIV,DEPT BIOL,COLLEGE STN,TX 77843
关键词
D O I
暂无
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
The inability to identify fragile sites from data for single individuals remains the major obstacle to determining whether these chromosomal loci are predisposed to cancer-causing and evolutionary rearrangements. We describe a novel statistical model that is amenable to data from single individuals and that establishes site-specific chromosomal breakage as nonrandom with respect to the distribution of total breakage. Our method tests incrementally smaller subsets of the data for homogeneity under a multinomial model that assigns equal probabilites to a maximal set of nonfragile sites and unrestricted probabilities to the remaining fragile sites with significantly higher numbers of breaks. We show how standardized Pearson's chi-square (Y-2) and likelihood-ratio (G(2)) Statistics can be appropriately used to measure goodness-of-fit for sparse contingency (individual-based) data in this model. A sample application of this approach indicates extensive variation in fragile sites among individuals and marked differences in fragile-site inferences from pooled as opposed to per-individual data.
引用
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页码:249 / 256
页数:8
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