Kenneth Kidd, PhD
Professor Emeritus of GeneticsCards
About
Research
Overview
Normal DNA sequence variation such as single nucleotide
polymorphisms (SNPs), short tandem repeat polymorphisms (STRPs), etc.
have made Homo sapiens amenable to many types of genetic analysis. We
are using these polymorphisms to study the genes for several
inherited disorders, including neuropsychiatric disorders, and working
on statistical methods to analyze the data. We are studying these and other
polymorphisms genome-wide on DNA samples from many different human populations with
an emphasis on understanding the organization of normal variation
including studies of linkage disequilibrium and estimates of the
distribution of the variation in the entire species. We have
established a database, ALFRED, the ALelle FREquency Database, to
accumulate allele frequencies of DNA polymorphisms. A current focus is on forensic uses of SNPs.
For the past several years my laboratory has studied the genetics of complex human disorders, those disorders that fail to show a Mendelian pattern but do "run in families". DNA polymorphisms are now being used to search for the genetic loci of major effect in behavioral and other complex disorders. Our previous efforts focused on finding genes responsible for neuropsychiatric disorders, especially Giles de la Tourette Syndrome and schizophrenia. While no locus appears to account for all cases of Tourette Syndrome, we have strong evidence of a predisposing genetic factor on the distal long arm of chromosome 17. Studies are ongoing through collaborations to narrow the region and identify the relevant variant.
We are studying the population genetics of expressed and non-expressed genetic variation at several genes of known neurologic relevance, such as the dopamine receptors D2 and D4 and the enzyme COMT, Catechol-O-methyl transferase. Also, because of their demonstrated relevance to alcoholism we are studying the genes involved in ethanol metabolism, the ADH genes and ALDH2. Understanding the nature of the common normal variation at these loci provides a background for investigating how they might influence normal and abnormal neurologic/metabolic function and susceptibility to psychiatric disorders. The duplicated ADH Class 1 genes are unique to primates and are the focus of molecular evolution studies. Several more evolution-oriented projects are also being pursued. These include theoretical studies as well as studying samples from diverse human populations for DNA polymorphisms. For some genes of interest we are also collecting DNA sequence of other great apes to examine the origins of the human lineage.
The lab's efforts are currently focused on genome diversity among world populations and understanding how that diversity arose. We have accumulated cell lines on individuals from over 45 different populations and plan to increase this resource in the coming years. On a global basis we are finding that the majority of alleles for nuclear DNA polymorphisms are present in most populations around the world, though sub-Saharan African populations have more genetic variation (alleles), in general, than indigenous populations in any other part of the world. We interpret the data to mean that there was a major founder effect and loss of variation associated with the expansion of modern humans out of Africa. Haplotype data collected on all of the populations we are studying are beginning to reveal patterns that provide a better understanding of that founder effect and the recent evolutionary history of modern humans. Recent studies have used these resources to select SNPs that can be useful in forensics, both for individual identification (matching the DNA at a crime scene with a suspect's DNA). Other SNPs are being selected for their value in inference of ancestry from an individual's DNA.
Bioinformatics research, in collaboration with the Yale Center for Medical Informatics, is ongoing in two areas. We are working to improve data management for the extensive marker typing results accumulating on many of the projects. We are also working to improve the utility of data in ALFRED through new search and display modes as well as relevant links to other online sources
For the past several years my laboratory has studied the genetics of complex human disorders, those disorders that fail to show a Mendelian pattern but do "run in families". DNA polymorphisms are now being used to search for the genetic loci of major effect in behavioral and other complex disorders. Our previous efforts focused on finding genes responsible for neuropsychiatric disorders, especially Giles de la Tourette Syndrome and schizophrenia. While no locus appears to account for all cases of Tourette Syndrome, we have strong evidence of a predisposing genetic factor on the distal long arm of chromosome 17. Studies are ongoing through collaborations to narrow the region and identify the relevant variant.
We are studying the population genetics of expressed and non-expressed genetic variation at several genes of known neurologic relevance, such as the dopamine receptors D2 and D4 and the enzyme COMT, Catechol-O-methyl transferase. Also, because of their demonstrated relevance to alcoholism we are studying the genes involved in ethanol metabolism, the ADH genes and ALDH2. Understanding the nature of the common normal variation at these loci provides a background for investigating how they might influence normal and abnormal neurologic/metabolic function and susceptibility to psychiatric disorders. The duplicated ADH Class 1 genes are unique to primates and are the focus of molecular evolution studies. Several more evolution-oriented projects are also being pursued. These include theoretical studies as well as studying samples from diverse human populations for DNA polymorphisms. For some genes of interest we are also collecting DNA sequence of other great apes to examine the origins of the human lineage.
The lab's efforts are currently focused on genome diversity among world populations and understanding how that diversity arose. We have accumulated cell lines on individuals from over 45 different populations and plan to increase this resource in the coming years. On a global basis we are finding that the majority of alleles for nuclear DNA polymorphisms are present in most populations around the world, though sub-Saharan African populations have more genetic variation (alleles), in general, than indigenous populations in any other part of the world. We interpret the data to mean that there was a major founder effect and loss of variation associated with the expansion of modern humans out of Africa. Haplotype data collected on all of the populations we are studying are beginning to reveal patterns that provide a better understanding of that founder effect and the recent evolutionary history of modern humans. Recent studies have used these resources to select SNPs that can be useful in forensics, both for individual identification (matching the DNA at a crime scene with a suspect's DNA). Other SNPs are being selected for their value in inference of ancestry from an individual's DNA.
Bioinformatics research, in collaboration with the Yale Center for Medical Informatics, is ongoing in two areas. We are working to improve data management for the extensive marker typing results accumulating on many of the projects. We are also working to improve the utility of data in ALFRED through new search and display modes as well as relevant links to other online sources
- Gene study using polymorphism of the DNA for several inherited disorders
- Collaborative study to narrow the region and identify the chromosome involved in Tourette syndrome and Schizophrenia
- Population genetics of expressed and non-expressed genetic variation at several genes of known neurologic relevance
- Bioinformatics research to improve data management for extensive marker typing results and improve the utility of data in ALFRED
Medical Research Interests
Africa; China; Gambia; Genetics; Global Health; India; Neuropsychiatry; Psychiatry
Academic Achievements & Community Involvement
News
News
- March 17, 2020Source: Validation of novel forensic DNA markers using multiplex microhaplotype sequencing
Validation of novel forensic DNA markers using multiplex microhaplotype sequencing
- April 24, 2018Source: Yale Daily News
Researchers discover a gene linked to language
- May 08, 2015
Written in blood
- May 15, 2014
Yale researchers identify gene that causes obesity-related metabolic syndrome