Extensive normal copy number variation of a beta-defensin antimicrobial-gene cluster
- PMID: 12916016
- PMCID: PMC1180683
- DOI: 10.1086/378157
Extensive normal copy number variation of a beta-defensin antimicrobial-gene cluster
Abstract
Using a combination of multiplex amplifiable probe hybridization and semiquantitative fluorescence in situ hybridization (SQ-FISH), we analyzed DNA copy number variation across chromosome band 8p23.1, a region that is frequently involved in chromosomal rearrangements. We show that a cluster of at least three antimicrobial beta-defensin genes (DEFB4, DEFB103, and DEFB104) at 8p23.1 are polymorphic in copy number, with a repeat unit >/=240 kb long. Individuals have 2-12 copies of this repeat per diploid genome. By segregation, microsatellite dosage, and SQ-FISH chromosomal signal intensity ratio analyses, we deduce that individual chromosomes can have one to eight copies of this repeat unit. Chromosomes with seven or eight copies of this repeat unit are identifiable by cytogenetic analysis as a previously described 8p23.1 euchromatic variant. Analysis of RNA from different individuals by semiquantitative reverse-transcriptase polymerase chain reaction shows a significant correlation between genomic copy number of DEFB4 and levels of its messenger RNA (mRNA) transcript. The peptides encoded by these genes are potent antimicrobial agents, especially effective against clinically important pathogens, such as Pseudomonas aeruginosa and Staphylococcus aureus, and DEFB4 has been shown to act as a cytokine linking the innate and adaptive immune responses. Therefore, a copy number polymorphism involving these genes, which is reflected in mRNA expression levels, is likely to have important consequences for immune system function.
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References
Electronic-Database Information
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- Fondation Jean Dausset–CEPH, http://www.cephb.fr/ (for marker database)
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- GenBank, http://www.ncbi.nlm.nih.gov/Genbank/ (for EPEV-1 [accession number BK001119], SCb-295j18 [accession number AF252830], and MAPH probes A [accession number NM_001147], B [accession number AF287957], C [accession number Z45294], D [accession number AF233439], E [accession number AF238378], F [accession number AC252830], G [accession number NM_04942], H [accession number G13705], I [accession number AA687243], J [accession number AA226797], K [accession number AA010611], L [accession number Z24258], M [accession number L34357], and N [accession number AQ318792])
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- GNF Gene Expression Atlas, http://expression.gnf.org/cgi-bin/index.cgi
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- Multiplex Amplifiable Probe Hybridization, http://www.nottingham.ac.uk/~pdzjala/maph/maph.html
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- Online Mendelian Inheritance in Man (OMIM), http://www.ncbi.nlm.nih.gov/Omim/ (for DEFB4, DEFB103, SPAG11, and CF)
References
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- Ausubel F, Brent R, Kingston RE, Moore DD, Seidman JG, Smith JA, Struhl K (eds) (1997) Short protocols in molecular biology. Wiley, New York
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- Bailey JA, Gu Z, Clark RA, Reinert K, Samonte RV, Schwartz S, Adams MD, Myers EW, Li PW, Eichler EE (2002) Recent segmental duplications in the human genome. Science 297:1003–1007 - PubMed
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