Applicability of a “Speed” Congenic Strategy to Dissect Blood Pressure Quantitative Trait Loci on Rat Chromosome 2 | Zendy

Baxter Jeffs | Zendy; Cervantes D. Negrín | Zendy; Delyth Graham | Zendy; James S. Clark | Zendy; Niall Anderson | Zendy; Dominique Gauguier | Zendy; Anna F. Dominiczak | Zendy

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Applicability of a “Speed” Congenic Strategy to Dissect Blood Pressure Quantitative Trait Loci on Rat Chromosome 2

Author(s) -

Baxter Jeffs,

Cervantes D. Negrín,

Delyth Graham,

James S. Clark,

Niall Anderson,

Dominique Gauguier,

Anna F. Dominiczak

Publication year - 2000

Publication title -

hypertension

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.986

H-Index - 265

eISSN - 1524-4563

pISSN - 0194-911X

DOI - 10.1161/01.hyp.35.1.179

Subject(s) - congenic , quantitative trait locus , biology , genetics , locus (genetics) , loss of heterozygosity , chromosome , backcrossing , introgression , gene , blood pressure , genetic marker , allele , endocrinology

The identification of any quantitative trait locus (QTL) via a genome scan is only the first step toward the ultimate goal of gene identification. The next step is the production of congenic strains by which the existence of a QTL may be verified and the implicated chromosomal region be reduced to a size applicable to positional cloning of the causal gene. We used a speed congenic breeding protocol previously verified in mice for 2 blood pressure QTLs on rat chromosome 2. Four congenic strains were produced through introgression of various segments of chromosome 2 from Wistar-Kyoto rats from Glasgow colonies [WKY((Gla)) rats] into the recipient stroke-prone spontaneously hypertensive rats from Glasgow colonies [SHRSP((Gla))], and vice versa. The number of backcross generations required for each strain to achieve complete homozygosity at 83 background genetic markers in a "best" male varied between 3 and 4. Transfer of the region of rat chromosome 2 containing both QTLs from WKY((Gla)) into an SHRSP((Gla)) genetic background lowered both baseline and salt-loaded systolic blood pressure by approximately 20 and approximately 40 mm Hg in male congenic rats compared with the SHRSP parental strain (F=53.4, P<0.005; F=28.0, P< 0.0005, respectively). In contrast, control animals for stowaway heterozygosity presented no deviation from the blood pressure values recorded for the SHRSP((Gla)), indicating that if such heterozygosity exists, its effect on blood pressure is negligible. A reciprocal strategy in which 1 or both QTLs on rat chromosome 2 were transferred from SHRSP((Gla)) into a WKY((Gla)) genetic background resulted in statistically significant but smaller blood pressure increases for 1 of these QTLs. These results confirm the existence of blood pressure QTLs on rat chromosome 2 and demonstrate the applicability of a speed congenic strategy in the rat and emphasize the important role of the genetic background.

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