Abstract

Positional cloning (also known as long-range cloning) refers to the process of identifying a gene by first determining its chromosomal location, and then isolating and screaming candidate genes from that region to isolate the specific gene. In the positional cloning projects described in this program, the chromosomal locations of the human and mouse loci of interest have been determined in the individual projects using genetic mapping techniques. Once the map position is sufficiently narrow, the strategy for isolation of the underlying gene is largely similar for the different genes, and is outlined in Fig.1. First, the region defined by genetic mapping is isolated in the form of large insert DNA clones. This is accomplished by screening libraries that carry large genomic DNA inserts, typically in the form of YAC (yeast artificial chromosome), BAC (bacterial artificial chromosome), and PAC (bacteriophage PI artificial chromosome) clones. Next, physical mapping of the clones is performed to determine clone insert size, overlap between inserts, and interclone distance. The goal is to cover the critical gene region with contiguous overlapping clones to produce a DNA 'contig' that contains the gene of the critical gene region with contiguous overlapping clones to produce a DNA 'contig' that contains the gene of interest. Various methods may then be employed to screen individual clones in the contig for the presence of the gene. The strategy used at this stage is dependent on properties of the specific mutation; one of the most powerful approaches, which will be used in multiple projects, is complementation of the mutant phenotype. Once a single genomic clone has been identified, efforts focus on identification of transcribed gene sequences using techniques such as direct cDNA selection, exon trapping and random sequencing. Finally, candidate genes identified from such as direct cDNA selection, exon trapping and random sequencing. Finally, candidate genes identified from the genomic region are evaluated by sequencing the corresponding gene to identify the mutation at the nucleotide.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL028481-18
Application #
6564849
Study Section
Project Start
2002-01-01
Project End
2002-12-31
Budget Start
Budget End
Support Year
18
Fiscal Year
2002
Total Cost
$234,836
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
119132785
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Lang, Jennifer M; Pan, Calvin; Cantor, Rita M et al. (2018) Impact of Individual Traits, Saturated Fat, and Protein Source on the Gut Microbiome. MBio 9:
Cherlin, Svetlana; Wang, Maggie Haitian; Bickeböller, Heike et al. (2018) Detecting responses to treatment with fenofibrate in pedigrees. BMC Genet 19:64
Park, Shuin; Ranjbarvaziri, Sara; Lay, Fides D et al. (2018) Genetic Regulation of Fibroblast Activation and Proliferation in Cardiac Fibrosis. Circulation 138:1224-1235
Roberts, Adam B; Gu, Xiaodong; Buffa, Jennifer A et al. (2018) Development of a gut microbe-targeted nonlethal therapeutic to inhibit thrombosis potential. Nat Med 24:1407-1417
Zhu, W; Buffa, J A; Wang, Z et al. (2018) Flavin monooxygenase 3, the host hepatic enzyme in the metaorganismal trimethylamine N-oxide-generating pathway, modulates platelet responsiveness and thrombosis risk. J Thromb Haemost 16:1857-1872
Lee, Jessica M; Ong, Jessica R; Vergnes, Laurent et al. (2018) Diet1, bile acid diarrhea, and FGF15/19: mouse model and human genetic variants. J Lipid Res 59:429-438
Miao, Zong; Alvarez, Marcus; Pajukanta, Päivi et al. (2018) ASElux: an ultra-fast and accurate allelic reads counter. Bioinformatics 34:1313-1320
Kurt, Zeyneb; Barrere-Cain, Rio; LaGuardia, Jonnby et al. (2018) Tissue-specific pathways and networks underlying sexual dimorphism in non-alcoholic fatty liver disease. Biol Sex Differ 9:46
Orozco, Luz D; Farrell, Colin; Hale, Christopher et al. (2018) Epigenome-wide association in adipose tissue from the METSIM cohort. Hum Mol Genet 27:1830-1846
Chella Krishnan, Karthickeyan; Kurt, Zeyneb; Barrere-Cain, Rio et al. (2018) Integration of Multi-omics Data from Mouse Diversity Panel Highlights Mitochondrial Dysfunction in Non-alcoholic Fatty Liver Disease. Cell Syst 6:103-115.e7

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