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Query: UMLS:C0028754 (
obesity
)
124,988
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
An overview of the status of the human obestiy gene map up to October 1995 is presented. The evidence is drawn from several lines of clinical and experimental research. First, 12 loci linked to
Mendelian disorders
exhibiting
obesity
as one clinical feature are reviewed. Second, six loci causing
obesity
in rodent models of the disease are considered. Third, eight chromosomal regions where quantitative trait loci, identified by crossbreeding experiments with informative strains of mice, are defined. Fourth, 10 candidate genes exhibiting a statistical association with BMI or body fat are introduced. Fifth, nine loci found to be linked to a relevant phenotype are listed and the four cases for which the evidence for linkage is strongest are emphasized. The latter are mapped to 2p25, 6p21.3, 7q33 and 20q12-13.11. Finally, the studies that have concluded that there was no association or linkage with a marker or gene are also reviewed. It is recommended that a system be developed by the
obesity
research community to ensure that an accurate and easily accessible computerized version of the human
obesity
gene map becomes available in the near future.
...
PMID:Current status of the human obesity gene map. 878 41
An update of the human
obesity
gene map up to October 1996 is presented. Evidence from
Mendelian disorders
exhibiting
obesity
as a clinical feature, single-gene mutation rodent models, quantitative trait loci uncovered in crossbreeding experiments with mouse, rat, and pig models, association and case-control studies with candidate genes, and linkage studies with genes and other markers is reviewed. All chromosomal locations of the animal loci are converted into human genome locations based on syntenic relationships between the genomes. A complete listing of all these loci reveals that only 4 of the 24 human chromosomes are not yet represented, i.e., 9, 18, 21, and Y. Several chromosome arms are characterized by the presence of several putative loci. The following arms include at least three such loci: 1p, 1q, 3p, 4q, 6p, 7q, 8p, 8q, 11p, 11q, 15q, 20q, and Xq. Studies with negative association and linkage results are also reviewed.
...
PMID:The human obesity gene map: the 1996 update. 906 16
An update of the human
obesity
gene map incorporating published results up to October 1997 is presented. Evidence from
Mendelian disorders
exhibiting
obesity
as a clinical feature; single-gene mutation rodent models; quantitative trait loci uncovered in human genome-wide scans and in crossbreeding experiments with mouse, rat, and pig models; association and case-control studies with candidate genes; and linkage studies with genes and other markers is reviewed. All chromosomal locations of the animal loci are converted into human genome locations based on syntenic relationships between the genomes. A complete listing of all of these loci reveals that all but chromosome Y of the 24 human chromosomes are represented. Some chromosomes show at least three putative loci related to
obesity
on both arms (1, 2, 6, 8, 11, and 20) and several on one chromosome arm only (3p, 4q, 5q, 7q, 12q, 13q, 15q, 15p, 22q, and Xq). Studies reporting negative association and linkage results are also listed, with the exception of the unlinked markers from genome-wide scans.
...
PMID:The human obesity gene map: the 1997 update. 952 74
An update of the human
obesity
gene map incorporating published results up to the end of October 1998 is presented. Evidence from the human
obesity
cases caused by single gene mutations; other
Mendelian disorders
exhibiting
obesity
as a clinical feature; quantitative trait loci uncovered in human genome-wide scans and in crossbreeding experiments with mouse, rat, and pig models; association and case-control studies with candidate genes; and linkage studies with genes and other markers is reviewed. The most noticeable changes from the 1997 update is the number of
obesity
cases due to single gene mutations that increased from three cases due to mutations in two genes to 25 cases due to 12 mutations in seven genes. A look at the
obesity
gene map depicted in Figure 1 reveals that putative loci affecting
obesity
-related phenotypes are found on all but chromosome Y of the human chromosomes. Some chromosomes show at least three putative loci related to
obesity
on both arms (1, 2, 3, 6, 7, 8, 9, 11, 17, 19, 20, and X) and several on one chromosome arm only (4q, 5q, 10q, 12q, 13q, 15q, 16p, and 22q). The number of genes and other markers that have been associated or linked with human
obesity
phenotypes is increasing very rapidly and now approaches 200.
...
PMID:The human obesity gene map: the 1998 update. 1002 38
This report constitutes the sixth update of the human
obesity
gene map incorporating published results up to the end of October 1999. Evidence from the rodent and human
obesity
cases caused by single gene mutations,
Mendelian disorders
exhibiting
obesity
as a clinical feature, quantitative trait loci (QTL) uncovered in human genome-wide scans and in crossbreeding experiments with mouse, rat, pig and chicken models, association and linkage studies with candidate genes and other markers is reviewed. Twenty-five human cases of
obesity
can now be explained by variation in five genes. Twenty
Mendelian disorders
exhibiting
obesity
as one of their clinical manifestations have now been mapped. The number of different QTLs reported from animal models reaches now 98. Attempts to relate DNA sequence variation in specific genes to
obesity
phenotypes continue to grow, with 89 reports of positive associations pertaining to 40 candidate genes. Finally, 44 loci have linked to
obesity
indicators in genomic scans and other linkage study designs. The
obesity
gene map depicted in Figure 1 reveals that putative loci affecting
obesity
-related phenotypes can be found on all autosomes, with chromosomes 14 and 21 showing each one locus only. The number of genes, markers, and chromosomal regions that have been associated or linked with human
obesity
phenotypes continues to increase and is now well above 200.
...
PMID:The human obesity gene map: the 1999 update. 1067 63
This report constitutes the seventh update of the human
obesity
gene map incorporating published results up to the end of October 2000. Evidence from the rodent and human
obesity
cases caused by single-gene mutations,
Mendelian disorders
exhibiting
obesity
as a clinical feature, quantitative trait loci uncovered in human genome-wide scans and in cross-breeding experiments in various animal models, and association and linkage studies with candidate genes and other markers are reviewed. Forty-seven human cases of
obesity
caused by single-gene mutations in six different genes have been reported in the literature to date. Twenty-four
Mendelian disorders
exhibiting
obesity
as one of their clinical manifestations have now been mapped. The number of different quantitative trait loci reported from animal models currently reaches 115. Attempts to relate DNA sequence variation in specific genes to
obesity
phenotypes continue to grow, with 130 studies reporting positive associations with 48 candidate genes. Finally, 59 loci have been linked to
obesity
indicators in genomic scans and other linkage study designs. The
obesity
gene map reveals that putative loci affecting
obesity
-related phenotypes can be found on all chromosomes except chromosome Y. A total of 54 new loci have been added to the map in the past 12 months and the number of genes, markers, and chromosomal regions that have been associated or linked with human
obesity
phenotypes is now above 250. Likewise, the number of negative studies, which are only partially reviewed here, is also on the rise.
...
PMID:The human obesity gene map: the 2000 update. 1131 48
A primary challenge in biomedical research today is the elucidation of the underlying genetic architecture of complex conditions such as
obesity
. In contrast to simple
Mendelian disorders
that result from a mutation in a single gene, complex phenotypes are the product of the action (as well as interaction) of multiple genes and environmental factors. The genetic configuration of these genes can range from effectively polygenic (i.e., many genes each with a relatively small contribution) to oligogenic (i.e., a few genes with relatively large measurable effects often expressed on a residual additive genetic background). While the task at hand is complicated, it is not intractable; however, it does require consideration of the nature of the disease and definition of its associated phenotypes in selecting the most appropriate study design. Here we will discuss the characteristics of
obesity
and its related phenotypes, which must be considered in designing analyses to identify the genes involved as well as reviewing what these approaches have provided in the search for genes influencing adiposity in humans
...
PMID:Searching for genes underlying normal variation in human adiposity. 1132 4
This report constitutes the eighth update of the human
obesity
gene map, incorporating published results up to the end of October 2001. Evidence from the rodent and human
obesity
cases caused by single-gene mutations,
Mendelian disorders
exhibiting
obesity
as a clinical feature, quantitative trait loci (QTLs) uncovered in human genome-wide scans and in crossbreeding experiments in various animal models, association and linkage studies with candidate genes and other markers is reviewed. The human cases of
obesity
related in some way to single-gene mutations in six different genes are incorporated. Twenty-five
Mendelian disorders
exhibiting
obesity
as one of their clinical manifestations have now been mapped. The number of different QTLs reported from animal models currently reaches 165. Attempts to relate DNA sequence variation in specific genes to
obesity
phenotypes continue to grow, with 174 studies reporting positive associations with 58 candidate genes. Finally, 59 loci have been linked to
obesity
indicators in genomic scans and other linkage study designs. The
obesity
gene map depicted in Figure 1 reveals that putative loci affecting
obesity
-related phenotypes can be found on all chromosomes except chromosome Y. A total of 54 new loci have been added to the map in the past 12 months, and the number of genes, markers, and chromosomal regions that have been associated or linked with human
obesity
phenotypes is now above 250. Likewise, the number of negative studies, which are only partially reviewed here, is also on the rise.
...
PMID:The human obesity gene map: the 2001 update. 1188 43
This is the ninth update of the human
obesity
gene map, incorporating published results through October 2002 and continuing the previous format. Evidence from single-gene mutation
obesity
cases,
Mendelian disorders
exhibiting
obesity
as a clinical feature, quantitative trait loci (QTLs) from human genome-wide scans and various animal crossbreeding experiments, and association and linkage studies with candidate genes and other markers is reviewed. For the first time, transgenic and knockout murine models exhibiting
obesity
as a phenotype are incorporated (N = 38). As of October 2002, 33 Mendelian syndromes relevant to human
obesity
have been mapped to a genomic region, and the causal genes or strong candidates have been identified for 23 of these syndromes. QTLs reported from animal models currently number 168; there are 68 human QTLs for
obesity
phenotypes from genome-wide scans. Additionally, significant linkage peaks with candidate genes have been identified in targeted studies. Seven genomic regions harbor QTLs replicated among two to five studies. Attempts to relate DNA sequence variation in specific genes to
obesity
phenotypes continue to grow, with 222 studies reporting positive associations with 71 candidate genes. Fifteen such candidate genes are supported by at least five positive studies. The
obesity
gene map shows putative loci on all chromosomes except Y. More than 300 genes, markers, and chromosomal regions have been associated or linked with human
obesity
phenotypes. The electronic version of the map with links to useful sites can be found at http://obesitygene.pbrc.edu.
...
PMID:The human obesity gene map: the 2002 update. 1263 30
Unlike simple rare
Mendelian disorders
, the genetic basis for common disorders is unclear. A general model of the genetics of common complex disorders is proposed which emphasizes the shared nature of common alleles in related common disorders, such as schizophrenia and bipolar disorder, Type II diabetes and
obesity
, and among autoimmune diseases. This model, the common variants/multiple disease hypothesis, emphasizes that many disease genes may not be disease specific. Common deleterious alleles, found at a relatively high frequency in the population may play a role in related clinical phenotypes in the context of different genetic backgrounds and under different environmental conditions.
...
PMID:The common variants/multiple disease hypothesis of common complex genetic disorders. 1496 46
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