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[title] => [Positional cloning of "Lisch-Like", a candidate modifier of susceptibility to type 2 diabetes in mice.]
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Dokmanovic-Chouinard+M">Dokmanovic-Chouinard M , Chung WK , Chevre JC , Watson E , Yonan J , Wiegand B , Bromberg Y , Wakae N , Wright CV , Overton J , Ghosh S , Sathe GM , Ammala CE , Brown KK , Ito R , LeDuc C , Solomon K , Fischer SG , Leibel RL ,</a></div>
<div class="biblio_source"><h3>Source: </h3> PLoS genetics, Volume 4, p.e1000137 (2008)</div>
<h3>URL:</h3><a href="http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137">http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137</a>
<h3>Abstract:</h3> <p>In 404 Lep(ob/ob) F2 progeny of a C57BL/6J (B6) x DBA/2J (DBA) intercross, we mapped a DBA-related quantitative trait locus (QTL) to distal Chr1 at 169.6 Mb, centered about D1Mit110, for diabetes-related phenotypes that included blood glucose, HbA1c, and pancreatic islet histology. The interval was refined to 1.8 Mb in a series of B6.DBA congenic/subcongenic lines also segregating for Lep(ob). The phenotypes of B6.DBA congenic mice include reduced beta-cell replication rates accompanied by reduced beta-cell mass, reduced insulin/glucose ratio in blood, reduced glucose tolerance, and persistent mild hypoinsulinemic hyperglycemia. Nucleotide sequence and expression analysis of 14 genes in this interval identified a predicted gene that we have designated "Lisch-like" (Ll) as the most likely candidate. The gene spans 62.7 kb on Chr1qH2.3, encoding a 10-exon, 646-amino acid polypeptide, homologous to Lsr on Chr7qB1 and to Ildr1 on Chr16qB3. The largest isoform of Ll is predicted to be a transmembrane molecule with an immunoglobulin-like extracellular domain and a serine/threonine-rich intracellular domain that contains a 14-3-3 binding domain. Morpholino knockdown of the zebrafish paralog of Ll resulted in a generalized delay in endodermal development in the gut region and dispersion of insulin-positive cells. Mice segregating for an ENU-induced null allele of Ll have phenotypes comparable to the B.D congenic lines. The human ortholog, C1orf32, is in the middle of a 30-Mb region of Chr1q23-25 that has been repeatedly associated with type 2 diabetes. </p>
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[biblio_authors] => [Dokmanovic-Chouinard M , Chung WK , Chevre JC , Watson E , Yonan J , Wiegand B , Bromberg Y , Wakae N , Wright CV , Overton J , Ghosh S , Sathe GM , Ammala CE , Brown KK , Ito R , LeDuc C , Solomon K , Fischer SG , Leibel RL ,]
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[biblio_abst_e] => [<p>In 404 Lep(ob/ob) F2 progeny of a C57BL/6J (B6) x DBA/2J (DBA) intercross, we mapped a DBA-related quantitative trait locus (QTL) to distal Chr1 at 169.6 Mb, centered about D1Mit110, for diabetes-related phenotypes that included blood glucose, HbA1c, and pancreatic islet histology. The interval was refined to 1.8 Mb in a series of B6.DBA congenic/subcongenic lines also segregating for Lep(ob). The phenotypes of B6.DBA congenic mice include reduced beta-cell replication rates accompanied by reduced beta-cell mass, reduced insulin/glucose ratio in blood, reduced glucose tolerance, and persistent mild hypoinsulinemic hyperglycemia. Nucleotide sequence and expression analysis of 14 genes in this interval identified a predicted gene that we have designated "Lisch-like" (Ll) as the most likely candidate. The gene spans 62.7 kb on Chr1qH2.3, encoding a 10-exon, 646-amino acid polypeptide, homologous to Lsr on Chr7qB1 and to Ildr1 on Chr16qB3. The largest isoform of Ll is predicted to be a transmembrane molecule with an immunoglobulin-like extracellular domain and a serine/threonine-rich intracellular domain that contains a 14-3-3 binding domain. Morpholino knockdown of the zebrafish paralog of Ll resulted in a generalized delay in endodermal development in the gut region and dispersion of insulin-positive cells. Mice segregating for an ENU-induced null allele of Ll have phenotypes comparable to the B.D congenic lines. The human ortholog, C1orf32, is in the middle of a 30-Mb region of Chr1q23-25 that has been repeatedly associated with type 2 diabetes. </p>]
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Dokmanovic-Chouinard+M">Dokmanovic-Chouinard M , Chung WK , Chevre JC , Watson E , Yonan J , Wiegand B , Bromberg Y , Wakae N , Wright CV , Overton J , Ghosh S , Sathe GM , Ammala CE , Brown KK , Ito R , LeDuc C , Solomon K , Fischer SG , Leibel RL ,</a></div>
<div class="biblio_source"><h3>Source: </h3> PLoS genetics, Volume 4, p.e1000137 (2008)</div>
<h3>URL:</h3><a href="http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137">http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137</a>
<h3>Abstract:</h3> <p>In 404 Lep(ob/ob) F2 progeny of a C57BL/6J (B6) x DBA/2J (DBA) intercross, we mapped a DBA-related quantitative trait locus (QTL) to distal Chr1 at 169.6 Mb, centered about D1Mit110, for diabetes-related phenotypes that included blood glucose, HbA1c, and pancreatic islet histology. The interval was refined to 1.8 Mb in a series of B6.DBA congenic/subcongenic lines also segregating for Lep(ob). The phenotypes of B6.DBA congenic mice include reduced beta-cell replication rates accompanied by reduced beta-cell mass, reduced insulin/glucose ratio in blood, reduced glucose tolerance, and persistent mild hypoinsulinemic hyperglycemia. Nucleotide sequence and expression analysis of 14 genes in this interval identified a predicted gene that we have designated "Lisch-like" (Ll) as the most likely candidate. The gene spans 62.7 kb on Chr1qH2.3, encoding a 10-exon, 646-amino acid polypeptide, homologous to Lsr on Chr7qB1 and to Ildr1 on Chr16qB3. The largest isoform of Ll is predicted to be a transmembrane molecule with an immunoglobulin-like extracellular domain and a serine/threonine-rich intracellular domain that contains a 14-3-3 binding domain. Morpholino knockdown of the zebrafish paralog of Ll resulted in a generalized delay in endodermal development in the gut region and dispersion of insulin-positive cells. Mice segregating for an ENU-induced null allele of Ll have phenotypes comparable to the B.D congenic lines. The human ortholog, C1orf32, is in the middle of a 30-Mb region of Chr1q23-25 that has been repeatedly associated with type 2 diabetes. </p>
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<div class="biblio_authors"><h3>Authors:</h3> <a href="/biblio/author/Dokmanovic-Chouinard+M">Dokmanovic-Chouinard M , Chung WK , Chevre JC , Watson E , Yonan J , Wiegand B , Bromberg Y , Wakae N , Wright CV , Overton J , Ghosh S , Sathe GM , Ammala CE , Brown KK , Ito R , LeDuc C , Solomon K , Fischer SG , Leibel RL ,</a></div>
<div class="biblio_source"><h3>Source: </h3> PLoS genetics, Volume 4, p.e1000137 (2008)</div>
<h3>URL:</h3><a href="http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137">http://www.plosgenetics.org/article/info:doi/10.1371/journal.pgen.1000137</a>
<h3>Abstract:</h3> <p>In 404 Lep(ob/ob) F2 progeny of a C57BL/6J (B6) x DBA/2J (DBA) intercross, we mapped a DBA-related quantitative trait locus (QTL) to distal Chr1 at 169.6 Mb, centered about D1Mit110, for diabetes-related phenotypes that included blood glucose, HbA1c, and pancreatic islet histology. The interval was refined to 1.8 Mb in a series of B6.DBA congenic/subcongenic lines also segregating for Lep(ob). The phenotypes of B6.DBA congenic mice include reduced beta-cell replication rates accompanied by reduced beta-cell mass, reduced insulin/glucose ratio in blood, reduced glucose tolerance, and persistent mild hypoinsulinemic hyperglycemia. Nucleotide sequence and expression analysis of 14 genes in this interval identified a predicted gene that we have designated "Lisch-like" (Ll) as the most likely candidate. The gene spans 62.7 kb on Chr1qH2.3, encoding a 10-exon, 646-amino acid polypeptide, homologous to Lsr on Chr7qB1 and to Ildr1 on Chr16qB3. The largest isoform of Ll is predicted to be a transmembrane molecule with an immunoglobulin-like extracellular domain and a serine/threonine-rich intracellular domain that contains a 14-3-3 binding domain. Morpholino knockdown of the zebrafish paralog of Ll resulted in a generalized delay in endodermal development in the gut region and dispersion of insulin-positive cells. Mice segregating for an ENU-induced null allele of Ll have phenotypes comparable to the B.D congenic lines. The human ortholog, C1orf32, is in the middle of a 30-Mb region of Chr1q23-25 that has been repeatedly associated with type 2 diabetes. </p>
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