Gene identification using exon amplification on human chromosome 18q21: Implications for bipolar disorder

H. Chen; Y. Huo; S. Patel; X. Zhu; T. Swift-Scanlan; R. H. Reeves; R. DePaulo; C. A. Ross; M. G. McInnis

doi:10.1038/sj.mp.4000780

Gene identification using exon amplification on human chromosome 18q21: Implications for bipolar disorder

H. Chen, Y. Huo, S. Patel, X. Zhu, T. Swift-Scanlan, R. H. Reeves, R. DePaulo, C. A. Ross, M. G. McInnis

School of Medicine

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

We previously reported linkage between bipolar disorder and a region on human chromosome (HC) 18q21. To identify genes in this region, exon trapping was performed on cosmids isolated from an HC18-specific cosmid library (LL18NC02) using 47 sequence tagged site (STS) markers from 18q21 as hybridization probes. A total of 285 unique sequences (exons) were obtained from 850 sequenced clones. Homology searching of the databases using NCBI's BLAST algorithms revealed that 31 exons have identity to known genes and/or ESTs, seven are identical to regions of finished genomic sequences in the 18q21 region, 20 have significant similarity (>30% sequence identity) to genes from human and/or other species, 19 were repetitive sequences, and 208 sequences (72%) are novel. Seventy per cent of the trapped sequences were predicted to be derived from genes using library screening and RT-PCR analyses. This represents an initial stage in characterizing genes in a susceptibility region for further study in bipolar disorder or other diseases that map to this region.

Original language	English (US)
Pages (from-to)	502-509
Number of pages	8
Journal	Molecular psychiatry
Volume	5
Issue number	5
DOIs	https://doi.org/10.1038/sj.mp.4000780
State	Published - 2000

Keywords

Bipolar disorder
Chromosome 18
Exon trapping
Exons

ASJC Scopus subject areas

Molecular Biology
Cellular and Molecular Neuroscience
Psychiatry and Mental health

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10.1038/sj.mp.4000780

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title = "Gene identification using exon amplification on human chromosome 18q21: Implications for bipolar disorder",

abstract = "We previously reported linkage between bipolar disorder and a region on human chromosome (HC) 18q21. To identify genes in this region, exon trapping was performed on cosmids isolated from an HC18-specific cosmid library (LL18NC02) using 47 sequence tagged site (STS) markers from 18q21 as hybridization probes. A total of 285 unique sequences (exons) were obtained from 850 sequenced clones. Homology searching of the databases using NCBI's BLAST algorithms revealed that 31 exons have identity to known genes and/or ESTs, seven are identical to regions of finished genomic sequences in the 18q21 region, 20 have significant similarity (>30% sequence identity) to genes from human and/or other species, 19 were repetitive sequences, and 208 sequences (72%) are novel. Seventy per cent of the trapped sequences were predicted to be derived from genes using library screening and RT-PCR analyses. This represents an initial stage in characterizing genes in a susceptibility region for further study in bipolar disorder or other diseases that map to this region.",

keywords = "Bipolar disorder, Chromosome 18, Exon trapping, Exons",

author = "H. Chen and Y. Huo and S. Patel and X. Zhu and T. Swift-Scanlan and Reeves, {R. H.} and R. DePaulo and Ross, {C. A.} and McInnis, {M. G.}",

note = "Funding Information: This study is supported by the Theodore and Vada Stanley Foundation; NIH grants to CAR (MH50763), MGM (MH01088) and JRD (MH42243); and National Alliance for Research on Schizophrenia and Depression (NARSAD) grant (JRD, MGM). We thank Drs Russell L Margolis and Virginia Willower for critical reading of the manuscript. We also thank Dr Russell L Margolis and John Kleiderlain for providing us with a set of filter lifts of a cerebellum cDNA library, and Drs OC Stine and A Heinzer for YAC contig construction.",

year = "2000",

doi = "10.1038/sj.mp.4000780",

language = "English (US)",

volume = "5",

pages = "502--509",

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number = "5",

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T1 - Gene identification using exon amplification on human chromosome 18q21

T2 - Implications for bipolar disorder

AU - Chen, H.

AU - Huo, Y.

AU - Patel, S.

AU - Zhu, X.

AU - Swift-Scanlan, T.

AU - Reeves, R. H.

AU - DePaulo, R.

AU - Ross, C. A.

AU - McInnis, M. G.

N1 - Funding Information: This study is supported by the Theodore and Vada Stanley Foundation; NIH grants to CAR (MH50763), MGM (MH01088) and JRD (MH42243); and National Alliance for Research on Schizophrenia and Depression (NARSAD) grant (JRD, MGM). We thank Drs Russell L Margolis and Virginia Willower for critical reading of the manuscript. We also thank Dr Russell L Margolis and John Kleiderlain for providing us with a set of filter lifts of a cerebellum cDNA library, and Drs OC Stine and A Heinzer for YAC contig construction.

PY - 2000

Y1 - 2000

N2 - We previously reported linkage between bipolar disorder and a region on human chromosome (HC) 18q21. To identify genes in this region, exon trapping was performed on cosmids isolated from an HC18-specific cosmid library (LL18NC02) using 47 sequence tagged site (STS) markers from 18q21 as hybridization probes. A total of 285 unique sequences (exons) were obtained from 850 sequenced clones. Homology searching of the databases using NCBI's BLAST algorithms revealed that 31 exons have identity to known genes and/or ESTs, seven are identical to regions of finished genomic sequences in the 18q21 region, 20 have significant similarity (>30% sequence identity) to genes from human and/or other species, 19 were repetitive sequences, and 208 sequences (72%) are novel. Seventy per cent of the trapped sequences were predicted to be derived from genes using library screening and RT-PCR analyses. This represents an initial stage in characterizing genes in a susceptibility region for further study in bipolar disorder or other diseases that map to this region.

AB - We previously reported linkage between bipolar disorder and a region on human chromosome (HC) 18q21. To identify genes in this region, exon trapping was performed on cosmids isolated from an HC18-specific cosmid library (LL18NC02) using 47 sequence tagged site (STS) markers from 18q21 as hybridization probes. A total of 285 unique sequences (exons) were obtained from 850 sequenced clones. Homology searching of the databases using NCBI's BLAST algorithms revealed that 31 exons have identity to known genes and/or ESTs, seven are identical to regions of finished genomic sequences in the 18q21 region, 20 have significant similarity (>30% sequence identity) to genes from human and/or other species, 19 were repetitive sequences, and 208 sequences (72%) are novel. Seventy per cent of the trapped sequences were predicted to be derived from genes using library screening and RT-PCR analyses. This represents an initial stage in characterizing genes in a susceptibility region for further study in bipolar disorder or other diseases that map to this region.

KW - Bipolar disorder

KW - Chromosome 18

KW - Exon trapping

KW - Exons

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Gene identification using exon amplification on human chromosome 18q21: Implications for bipolar disorder

Abstract

Keywords

ASJC Scopus subject areas

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