TY - JOUR
T1 - Characterization of the murine Lbx2 promoter, identification of the human homologue, and evaluation as a candidate for Alström syndrome
AU - Chen, Fabian
AU - Collin, Gayle B.
AU - Liu, Kenneth C.
AU - Beier, David R.
AU - Eccles, Michael
AU - Nishina, Patsy M.
AU - Moshang, Thomas
AU - Epstein, Jonathan A.
N1 - Funding Information:
We acknowledge Douglas McMinimy (The Jackson Laboratory) for sequencing services. G.B.C. and P.M.N. were supported by NIH Grant HD36878 and an institutional shared service grant from the National Cancer Institute, CA-34196. This work was supported in part by the Cancer Society of New Zealand, and M.R.E. is a Royal Society of New Zealand Cook Fellow. This work was supported by the AHA, the W. W. Smith Charitable Trust, and NIH Grants RO1HL62974, RO1HL61475, and RO1DK57050 to J.A.E.
PY - 2001/6/1
Y1 - 2001/6/1
N2 - The murine Lbx2 gene is a member of the ladybird family of homeobox genes, which is expressed in the developing urogenital system, eye, and brain. Using transgenic mice, we demonstrate that 9 kb of the 5′ flanking region of mouse Lbx2 is able to direct expression of a reporter gene in a tissue-specific manner recapitulating the endogenous expression pattern. This regulatory region provides a novel reagent allowing for transgenic expression in the developing urogenital ridge. In addition, we describe the identification of the human homologue, LBX2. Comparison of the human LBX2 and mouse Lbx2 sequences upstream of the coding regions reveals sequence conservation suggesting conserved regulatory regions. Both the human LBX2 and the mouse Lbx2 genes have similar genomic structures and are composed of two exons separated by an intron. We mapped the mouse Lbx2 gene to 35 cM on chromosome 6 and the human LBX2 gene to a homologous region of chromosome 2p13. This is a candidate region for several inherited disorders, including Alström syndrome, a disorder that includes ocular, urogenital, and renal abnormalities. Given the expression pattern of Lbx2, the chromosomal location in humans, and the potential function of mammalian ladybird genes, we have begun to analyze patients with ocular disorders and those with Alström syndrome for mutations in LBX2. Although polymorphisms were identified, our results indicate that mutations in the coding region of LBX2 do not account for Alström syndrome in the six kindreds analyzed.
AB - The murine Lbx2 gene is a member of the ladybird family of homeobox genes, which is expressed in the developing urogenital system, eye, and brain. Using transgenic mice, we demonstrate that 9 kb of the 5′ flanking region of mouse Lbx2 is able to direct expression of a reporter gene in a tissue-specific manner recapitulating the endogenous expression pattern. This regulatory region provides a novel reagent allowing for transgenic expression in the developing urogenital ridge. In addition, we describe the identification of the human homologue, LBX2. Comparison of the human LBX2 and mouse Lbx2 sequences upstream of the coding regions reveals sequence conservation suggesting conserved regulatory regions. Both the human LBX2 and the mouse Lbx2 genes have similar genomic structures and are composed of two exons separated by an intron. We mapped the mouse Lbx2 gene to 35 cM on chromosome 6 and the human LBX2 gene to a homologous region of chromosome 2p13. This is a candidate region for several inherited disorders, including Alström syndrome, a disorder that includes ocular, urogenital, and renal abnormalities. Given the expression pattern of Lbx2, the chromosomal location in humans, and the potential function of mammalian ladybird genes, we have begun to analyze patients with ocular disorders and those with Alström syndrome for mutations in LBX2. Although polymorphisms were identified, our results indicate that mutations in the coding region of LBX2 do not account for Alström syndrome in the six kindreds analyzed.
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U2 - 10.1006/geno.2001.6539
DO - 10.1006/geno.2001.6539
M3 - Article
C2 - 11386758
AN - SCOPUS:0035366412
SN - 0888-7543
VL - 74
SP - 219
EP - 227
JO - Genomics
JF - Genomics
IS - 2
ER -