Characterization of the genomic structure and function of regions influencing renin and angiogenesis in the SS rat

Stodola, Timothy J.; Resende, Micheline; Sarkis, Allison B.; Didier, Daniela N.; Jacob, Howard J.; Huebner, Norbert; Hummel, Oliver; Saar, Kathrin; Moreno, Carol; Greene, Andrew S.

doi:10.1152/physiolgenomics.00171.2010

Cited by 8 publications

(18 citation statements)

References 69 publications

(86 reference statements)

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“…11 They reported that the SR Renin region increased BP (Δ+30 mmHg; P <0.05) in the SS-13 SR congenic (referred to as S/ren rr ) compared with SS (Figure 2A). 11 Also similar to line 9 13, 14 , the S/ren rr congenic restores plasma renin activity (PRA), 19 angiogenesis, 19 and vasoreactivity, 20 indicating that line 9 and S/ren rr share some functional allele(s), but not all. Most notably, the protective region around Renin (46.1–47.2 Mb) did not offset the hypertensive BP allele(s) in S/ren rr , 11 as was detected in line 9 (Figure 2).…”

Section: Resultsmentioning

confidence: 92%

“…We compared the SS/Jr (used by Jiang et al 11 ), the SS/JrMcwi (used for our SS-13 BN congenics 13 ), the SR, and the BN genomic sequences across the entire 3.7 Mb line 9 congenic interval to identify common and unique variants among the strains (Supplementary Table 2). Across the line 9 interval, only 2 variants (<0.0001%) were polymorphic between SS/Jr and SS/JrMcwi, and therefore, we hereafter use SS to denote both strains.…”

Section: Resultsmentioning

confidence: 99%

“…Combined, the SS had 267 variants that differed from both SR and BN, of which 1 nonsynonymous variant was predicted to be damaging. These common variants likely include shared SR and BN allele(s) that regulate renin expression, 13, 19 angiogenesis, 13, 19 and vasoreactivity 14, 20 that were restored in both line 9 and S/ren rr .…”

Section: Resultsmentioning

confidence: 99%

“…Genomic boundaries for congenic lines 9, 9A, 9B, and 9C were described previously, 13 but have been further refined here (Figure 1). …”

Section: Methodsmentioning

confidence: 96%

“…13–15 This revealed a protective region (chr13:46.1–47.2 Mb) promoting lower blood pressure (referred to as line9 BP1 ) that is offset by an adjacent region promoting higher blood pressure (chr13:47.2–49.0 Mb; referred to as line9 BP2 ), both derived from the same strain. We also reanalyzed archived DNA from the hypertensive S/ren rr congenic strain (SR Renin on a SS background) used in a 1996 study published in Hypertension by Jiang et al 11 This reduced by 85% the undefined congenic interval of S/ren rr , enabling us to compare overlapping sequence between SS, SR, and Brown Norway (BN) in our congenic region.…”

Section: Introductionmentioning

confidence: 99%

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Congenic Mapping and Sequence Analysis of the Renin Locus

et al. 2013

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Renin was the first blood pressure (BP) quantitative trait locus (QTL) mapped by linkage analysis in the rat. Subsequent BP linkage and congenic studies capturing different portions of the renin region have returned conflicting results, suggesting that multiple interdependent BP loci may be residing in the chromosome 13 BP QTL that includes Renin. We used SS-13BN congenic strains to map 2 BP loci in the Renin region (chr13:45.2–49.0 Mb). We identified a 1.1 Mb protective Brown Norway (BN) region around Renin (chr13:46.1–47.2 Mb) that significantly decreased BP by 32 mmHg. The Renin protective BP locus was offset by an adjacent hypertensive locus (chr13:47.2–49.0 Mb) that significantly increased BP by 29 mmHg. Sequence analysis of the protective and hypertensive BP loci revealed 1,433 and 2,063 variants between Dahl salt-sensitive/Mcwi (SS) and BN rats, respectively. To further reduce the list of candidate variants, we re-genotyped an overlapping SS-13SR congenic strain (S/renrr) with a previously reported BP phenotype. Sequence comparison between SS, Dahl R (SR), and BN reduced the number of candidate variants in the 2 BP loci by 42% for further study. Combined with previous studies, these data suggest that at least 4 BP loci reside within the 30 cM chromosome 13 BP QTL that includes Renin.

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Section: Resultsmentioning

confidence: 92%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

“…Genomic boundaries for congenic lines 9, 9A, 9B, and 9C were described previously, 13 but have been further refined here (Figure 1). …”

Section: Methodsmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Congenic Mapping and Sequence Analysis of the Renin Locus

et al. 2013

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Enhancement of Resting-State fcMRI Networks by Prior Sensory Stimulation

Ward

et al. 2014

Brain Connectivity

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It is important to consider the effect of a previous experimental condition when analyzing resting-state functional connectivity magnetic resonance imaging (fcMRI) data. In this work, a simple sensory stimulation functional MRI (fMRI) experiment was conducted between two resting-state fcMRI acquisitions in anesthetized rats using a high-field small-animal MR scanner. Previous human studies have reported fcMRI network alteration by prior task/stimulus utilizing similar experimental paradigms. An anesthetized rat preparation was used to test whether brain regions with higher level functions are involved in post-task/stimulus fcMRI network alteration. We demonstrate significant fcMRI enhancement poststimulation in the sensory cortical, limbic, and insular brain regions in rats. These brain regions have been previously implicated in vigilance and anesthetic arousal networks. We tested their experimental paradigm in several inbred strains of rats with known phenotypic differences in anesthetic susceptibility and cerebral vascular function. Brown Norway (BN), Dahl Salt-Sensitive (SS), and consomic SSBN13 strains were tested. We have previously shown significant differences in blood oxygen level-dependent fMRI activity and fcMRI networks across these strains. Here we report statistically significant interstrain differences in regional fcMRI poststimulation enhancement. In the SS strain, poststimulation enhancement occurred in posterior sensory and limbic cortical brain regions. In the BN strain, poststimulation enhancement appeared in anterior cingulate and subcortical limbic brain regions. These results imply that a prior condition has a significant impact on fcMRI networks that depend on intersubject difference in genetics and physiology.

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Targeting the endothelial progenitor cell surface proteome to identify novel mechanisms that mediate angiogenic efficacy in a rodent model of vascular disease

Kaczorowski

Stodola

Prisco

et al. 2013

Physiological Genomics

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Endothelial progenitor cells (EPCs) promote angiogenesis, and clinical trials suggest autologous EPC-based therapy may be effective in treatment of vascular diseases. Albeit promising, variability in the efficacy of EPCs associated with underlying disease states has hindered the realization of EPC-based therapy. Here we first identify and characterize EPC dysfunction in a rodent model of vascular disease (SS/Mcwi rat) that exhibits impaired angiogenesis. To identify molecular candidates that mediate the angiogenic potential of these cells, we performed a broad analysis of cell surface protein expression using chemical labeling combined with mass spectrometry. Analysis revealed EPCs derived from SS/Mcwi rats express significantly more type 2 low-affinity immunoglobulin Fc-gamma (FCGR2) and natural killer 2B4 (CD244) receptors compared with controls. Genome-wide sequencing (RNA-seq) and qt-PCR confirmed isoforms of CD244 and FCGR2a transcripts were increased in SS/Mcwi EPCs. EPCs with elevated expression of FCGR2a and CD244 receptors are predicted to increase the probability of SS/Mcwi EPCs being targeted for death, providing a mechanistic explanation for their reduced angiogenic efficacy in vivo. Pathway analysis supported this contention, as "key" molecules annotated to cell death paths were differentially expressed in the SS/Mcwi EPCs. We speculate that screening and neutralization of cell surface proteins that "tag" and impair EPC function may provide an alternative approach to utilizing incompetent EPCs in greater numbers, as circulating EPCs are depleted in patients with vascular disease. Overall, novel methods to identify putative targets for repair of EPCs using discovery-based technologies will likely provide a major advance in the field of regenerative medicine.

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Characterization of the genomic structure and function of regions influencing renin and angiogenesis in the SS rat

Cited by 8 publications

References 69 publications

Congenic Mapping and Sequence Analysis of the Renin Locus

Congenic Mapping and Sequence Analysis of the Renin Locus

Enhancement of Resting-State fcMRI Networks by Prior Sensory Stimulation

Targeting the endothelial progenitor cell surface proteome to identify novel mechanisms that mediate angiogenic efficacy in a rodent model of vascular disease

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