Single-nucleotide polymorphisms (SNPs) are rapidly replacing microsatellites as the markers of choice for genetic linkage studies and many other studies of human pedigrees. Here, we describe an efficient approach for modeling linkage disequilibrium (LD) between markers during multipoint analysis of human pedigrees. Using a gene-counting algorithm suitable for pedigree data, our approach enables rapid estimation of allele and haplotype frequencies within clusters of tightly linked markers. In addition, with the use of a hidden Markov model, our approach allows for multipoint pedigree analysis with large numbers of SNP markers organized into clusters of markers in LD. Simulation results show that our approach resolves previously described bia...
Certain human hereditary conditions, notably those with low penetrance and those which require an en...
In the 'indirect' method of detecting genetic associations between a trait and a DNA variant, we typ...
We present a novel approach to disease-gene mapping via cladistic analysis of single-nucleotide poly...
Lately, many different methods of linkage, association or joint analysis for family data have been i...
Dense sets of hundreds of thousands of markers have been developed for genome-wide association studi...
Dense sets of hundreds of thousands of markers have been developed for genome-wide association studi...
The genotyping of closely spaced single-nucleotide polymorphism (SNP) markers frequently yields high...
Several applications necessitate an unbiased determination of relatedness, be it in linkage or assoc...
The genotyping of closely spaced single-nucleotide polymorphism (SNP) markers frequently yields high...
SummaryMolecular geneticists are developing the third-generation human genome map with single-nucleo...
Computational constraints currently limit exact multipoint linkage analysis to pedigrees of moderate...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
This paper describes a likelihood based fine scale linkage disequilibrium mapping method for estimat...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
Certain human hereditary conditions, notably those with low penetrance and those which require an en...
In the 'indirect' method of detecting genetic associations between a trait and a DNA variant, we typ...
We present a novel approach to disease-gene mapping via cladistic analysis of single-nucleotide poly...
Lately, many different methods of linkage, association or joint analysis for family data have been i...
Dense sets of hundreds of thousands of markers have been developed for genome-wide association studi...
Dense sets of hundreds of thousands of markers have been developed for genome-wide association studi...
The genotyping of closely spaced single-nucleotide polymorphism (SNP) markers frequently yields high...
Several applications necessitate an unbiased determination of relatedness, be it in linkage or assoc...
The genotyping of closely spaced single-nucleotide polymorphism (SNP) markers frequently yields high...
SummaryMolecular geneticists are developing the third-generation human genome map with single-nucleo...
Computational constraints currently limit exact multipoint linkage analysis to pedigrees of moderate...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
This paper describes a likelihood based fine scale linkage disequilibrium mapping method for estimat...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
Single-marker linkage-disequilibrium (LD) methods cannot fully describe disequilibrium in an entire ...
Certain human hereditary conditions, notably those with low penetrance and those which require an en...
In the 'indirect' method of detecting genetic associations between a trait and a DNA variant, we typ...
We present a novel approach to disease-gene mapping via cladistic analysis of single-nucleotide poly...