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1. |
Renin-Angiotensin and Kallikrein-Kinin Systems Coordinately Modulate Angiogenesis |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 29-29
Costanza Emanueli,
Paolo Madeddu,
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ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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2. |
Genomewide Linkage Scan of Resting Blood PressureHERITAGE Family Study |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1037-1043
Treva Rice,
Tuomo Rankinen,
Yvon Chagnon,
Michael Province,
Louis Pérusse,
Arthur Leon,
James Skinner,
Jack Wilmore,
Claude Bouchard,
Dabeeru Rao,
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摘要:
The purpose of this study was to search for genomic regions influencing resting systolic (SBP) and diastolic (DBP) blood pressure (BP) in sedentary families (baseline), and for resting BP responses (changes) resulting from a 20-week exercise training intervention (post-training–baseline) in the Health, Risk Factors, Exercise Training, and Genetics (HERITAGE) Family Study. A genome-wide scan was conducted on 317 black individuals from 114 families and 519 white individuals from 99 families using a multipoint variance-components linkage model and a panel of 509 markers. Promising results were primarily, but not exclusively, found in the black families. Linkage evidence (P<0.0023) with baseline BP replicated other studies within a 1-logarithm of odds (LOD) interval on 2p14, 3p26.3, and 12q21.33, and provided new evidence on 3q28, 11q21, and 19p12. Results for several known hypertension genes were less compelling. For response BP, results were not very strong, although markers on 13q11 were mildly suggestive (P<0.01). In conclusion, these HERITAGE data, in conjunction with results from previous genomewide scans, provide a basis for planning future investigations. The major areas warranting further study involve fine mapping to narrow down 3 regions on 2q, 3p, and 12q that may contain “novel” hypertension genes, additional typing of some biological candidate genes to determine whether they are the sources of these and other signals, multilocus investigations to understand how and to what extent some of these candidates may interact, and multivariate studies to characterize any pleiotropy.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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3. |
Linkage of Essential Hypertension to Chromosome 18q |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1044-1049
Kristleifur Kristjansson,
Andrei Manolescu,
Arni Kristinsson,
Thordur Hardarson,
Helga Knudsen,
Sigurdur Ingason,
Gudmar Thorleifsson,
Michael Frigge,
Augustine Kong,
Jeffrey Gulcher,
Kari Stefansson,
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摘要:
We performed a genomewide scan with 904 microsatellite markers using 120 extended Icelandic families with 490 hypertensive patients. The families were identified by cross-matching a list of hypertensive patients from the Hypertension Clinic of the University Hospital (Landspitalinn) in Iceland with a genealogy database of the entire Icelandic nation. After adding 5 markers, we found linkage to chromosome 18q with an allele-sharing LOD score of 4.60 (P=2.1× 10−6). These results provide evidence for a novel susceptibility gene for essential hypertension on chromosome 18q and show that it is possible to study the genetics of essential hypertension without stratifying by subphenotypes.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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4. |
Conserved Synteny in Rat and Mouse for a Blood Pressure QTL on Human Chromosome 17 |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1050-1052
Heike Zimdahl,
Thomas Kreitler,
Claudia Gösele,
Detlev Ganten,
Norbert Hübner,
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摘要:
Evidence for blood pressure quantitative trait loci (QTLs) on rat chromosome 10 has been found in multiple independent studies. Analysis of the homologous region on human chromosome 17 revealed significant linkage to blood pressure. The critical segment on human chromosome 17 spans a large interval containing the genesItga2b, Gfap, andItgb3. Therefore, findings in the rat may help to refine the position of blood pressure–regulating loci, assuming a common molecular cause across species. However, it has recently been suggested that the gene order in human, rat, and mouse is not conserved in this region, leaving uncertainty about the overlap of the blood pressure– regulating region between human chromosome 17 and rat chromosome 10. We have performed a detailed comparative analysis among human, mouse, and rat, defining the segment in question, by obtaining gene structure information in silico and by radiation hybrid mapping. It is of interest that this region also containsWnk4, a gene previously identified to cause pseudohypoaldosteronism type II and human hypertension. Our results definitively show that the conserved synteny extends among human chromosome 17, rat chromosome 10, and mouse chromosome 11, demonstrating an overlap between previously localized blood pressure QTLs in humans and rats.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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5. |
ADD1460W Allele Associated With Cardiovascular Disease in Hypertensive Individuals |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1053-1057
Alanna Morrison,
Molly Bray,
Aaron Folsom,
Eric Boerwinkle,
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摘要:
High blood pressure is a predictor of cardiovascular disease. Hence, genes contributing to essential hypertension may play a role in the etiology of cardiovascular disease. For this reason, we examined the association between the &agr;-adducin (ADD1) G460W and G-protein &bgr;3 subunit (GNB3) 825C>T polymorphisms and the prevalence of peripheral arterial disease (PAD) and incidence of coronary heart disease (CHD) in non-Hispanic whites from the Atherosclerosis Risk in Communities (ARIC) Study. PAD prevalence was defined by an ankle-brachial index, ie, the ratio of ankle systolic blood pressure to brachial artery systolic blood pressure, of ≤0.90 for men and ≤0.85 for women. CHD incidence was determined by following the ARIC cohort for a median of 5.3 years for potential coronary events. Stratified random samples of the ARIC cohort (n=703 and n=684) were used, respectively, as the comparison groups for the PAD (n=144) and incident CHD (n=408) cases. TheGNB3825T allele and theADD1460W allele were not significantly associated with prevalence of PAD or incidence of CHD. However, a test of the interaction between hypertension status and theADD1G460W polymorphism indicated that further evaluation of theADD1polymorphism in only hypertensive individuals was warranted. TheADD1460W allele was significantly associated with PAD (odds ratio [OR]: 2.61, 95% CI, 1.27–5.37,P=0.01) and CHD (hazard rate ratio [HRR]: 2.30, 95% CI, 1.20–4.42,P=0.01) in hypertensive individuals after adjustment for multiple cardiovascular disease risk factors. An interaction with hypertension in the association between theADD1G460W polymorphism and cardiovascular disease merits further testing in additional populations.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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6. |
Myocyte Redistribution of GRK2 and GRK5 in Hypertensive, Heart-Failure–Prone Rats |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1058-1063
Xian Yi,
A. Gerdes,
Faqian Li,
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摘要:
G protein–coupled receptor kinases (GRKs) are known to be involved in the development of cardiac hypertrophy. Their exact role and subcellular distribution during cardiac hypertrophy and failure remain to be elucidated. We examined expression and subcellular distribution of GRK2 and GRK5 in the left ventricle of female spontaneously hypertensive heart failure (SHHF) rats at 6 months of age using Western blots and fluorescent confocal microscopy. GRK2 was expressed mainly in the Triton X-100 soluble fraction in the left ventricle with similar expression levels between SHHF and age-matched Wistar-Kyoto (WKY) rats. GRK2 had a striated pattern which colocalized with sarcomeric &agr;-actinin and G protein in both SHHF and WKY rat myocytes and specifically accumulated in the intercalated disks of myocytes from SHHF but not WKY rats. GRK5 was expressed in both the Triton X-100 soluble fraction and Triton X-100 insoluble fraction in the left ventricle with similar expression levels between SHHF and WKY rats. GRK5 distributed diffusely in the cytoplasm in both SHHF and WKY rat myocytes and specifically accumulated in the nucleus of myocytes from SHHF but not WKY rats. GRK5 colocalized with coilin, the major component of the nuclear substructure involved in RNA synthesis and processing. The results suggest different roles for GRK2 and GRK5 in G-protein signaling and RNA biogenesis. Subcellular redistribution of GRK2 and GRK5 may be involved in cardiac hypertrophy resulting from chronic hypertension.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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7. |
Urinary Protein and Essential Hypertension in Black and in White People |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1064-1070
Rajani Chelliah,
Giuseppe Sagnella,
Nirmala Markandu,
Graham MacGregor,
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摘要:
The objectives of this work were to examine the association between urinary protein and blood pressure and to compare the pattern of urinary protein excretion with essential hypertension in people of European origin (whites) and in people of African or African-Caribbean origin (blacks) living in southwest London, United Kingdom. In the groups as a whole, there were no significant differences in total urinary protein excretion between blacks and whites (geometric means [95% CI]: 94.0 [85.9 to 102.9] mg/24h for the blacks [n=151] and 102.1 [96.1 to 108.4] mg/24h for the whites [n= 219]). There were also no significant differences between blacks and whites in urinary albumin (6.5 [4.9 to 8.5] mg/24h for the blacks [n=97] and 7.1 [5.6 to 9.0] mg/24h for the whites [n=123]). In both groups, those with essential hypertension displayed a significantly raised urinary protein excretion (1.21-fold higher for the blacks and 1.19-fold higher for the whites) and albumin excretion (1.69-fold higher for the blacks and 2.40-fold higher for the whites). Urinary transferrin excretion measured in a subgroup of 67 subjects was also raised in those with essential hypertension (3.22-fold higher in the blacks and 2.76-fold higher in the whites). Examination of urinary proteins by SDS-PAGE did not identify any pattern consistent with a reduction in renal tubular protein reabsorption in those with essential hypertension. These results suggest that the increase in protein excretion in essential hypertension could be due, at least in part, to an increase in glomerular protein ultrafiltration.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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8. |
Fetal Uninephrectomy Leads to Postnatal Hypertension and Compromised Renal Function |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1071-1076
Karen Moritz,
E. Wintour,
Miodrag Dodic,
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摘要:
It has been proposed that the number of nephrons an individual has may be inversely related to his or her blood pressure. In this study using female ovine fetuses, nephron number was reduced by performing a fetal uninephrectomy during the period of active nephrogenesis (100 days of gestation, term=150 days). Lambs were born at term and grew at a similar rate. At 5 months of age, ovaries were removed and the carotid artery exteriorized into a fold of skin. Blood pressure and renal function were studied at 6 and 12 months of age. At 6 months of age, uninephrectomized lambs had significantly higher mean arterial blood pressure than sham-operated lambs (89±2 versus 82±2 mm Hg,P<0.05) when measured over a 3-day period. Heart rate was not different between the groups. Urine flow rate was similar, but glomerular filtration rate was significantly lower in uninephrectomized animals (P<0.05). Urinary concentrations and excretion rates of sodium tended to be higher in uninephrectomized animals but were similar for chloride and potassium. There was no evidence of proteinuria in the uninephrectomized lambs. Similar differences were observed in blood pressure and renal function at 12 months of age. Plasma renin concentrations at this age were lower in the uninephrectomized lambs (P<0.05). An oral salt load for 10 days did not increase blood pressure significantly in either group at 12 months of age, nor were there differences in the responsiveness to graded doses of angiotensin II. These results suggest that formation of a low nephron number in utero, may result in elevated blood pressure and compromised renal function in later life.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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9. |
Renoprotective Effect of Chronic Adrenomedullin Infusion in Dahl Salt-Sensitive Rats |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1077-1082
Toshio Nishikimi,
Yosuke Mori,
Naohiko Kobayashi,
Kazuyoshi Tadokoro,
Xin Wang,
Kazumi Akimoto,
Fumiki Yoshihara,
Kenji Kangawa,
Hiroaki Matsuoka,
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摘要:
The present study was designed to examine whether chronic adrenomedullin infusion has renoprotective effects in hypertensive renal failure and the mechanism by which chronic adrenomedullin infusion exerts its effects. Dahl salt-sensitive rats and Dahl salt-resistant rats were fed a high salt diet starting at 6 weeks of age. Recombinant human adrenomedullin or vehicle was infused for 7 weeks in 11-week-old Dahl salt-sensitive rats. Dahl salt-resistant rat was used as a control. After 7 weeks, untreated Dahl salt-sensitive rats were characterized by decreased kidney function, abnormal morphological findings, increased hormone levels, increased renal tissue angiotensin II levels, and altered mRNA expressions of transforming growth factor &bgr; (TGF-&bgr;) and components of the renin-angiotensin system compared with Dahl salt-resistant rats. Chronic adrenomedullin treatment significantly improved renal function (serum creatinine −87%, creatinine clearance +114%, urinary protein excretion −59%) and histological findings (glomerular injury score −54%) without changing mean arterial pressure compared with untreated Dahl salt-sensitive rats. Interestingly, long-term human adrenomedullin infusion decreased the endogenous rat adrenomedullin level (−97%) with a slight increase of human adrenomedullin level. Chronic adrenomedullin treatment also significantly inhibited the increase of plasma renin concentration (−269%), aldosterone level (−82%), and renal tissue angiotensin II levels (−60%). Furthermore, adrenomedullin infusion significantly decreased the increases of mRNA expressions of TGF-&bgr; (− 63%), angiotensin-converting enzyme (−137%), renin (−230%), and angiotensinogen (−38%) in renal cortex. These results suggest that increased endogenous adrenomedullin plays a compensatory role in chronic hypertensive renal failure and that long-term adrenomedullin infusion has renoprotective effects in this type of hypertension model, partly via inhibition of the circulating and renal renin-angiotensin system.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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10. |
Heart RateAn Important Confounder of Pulse Wave Velocity Assessment |
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Hypertension: Journal of The American Heart Association,
Volume 39,
Issue 6,
2002,
Page 1083-1087
Pierre Lantelme,
Christine Mestre,
Michel Lievre,
Alain Gressard,
Hugues Milon,
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摘要:
Arterial stiffness is a strong determinant of cardiovascular risk. Pulse wave velocity (PWV) is an index of arterial stiffness, and its prognostic value has been repeatedly emphasized. The purpose of the present study was to assess the effect of heart rate (HR) on PWV. Twenty-two subjects with a mean age of 77.8±8.4 (SD) years and permanent cardiac pacing were studied. In each subject, PWV was measured at 5 different pacing frequencies in the same session (60, 70, 80, 90, 100 bpm), the order of the various frequencies being randomly determined. Furthermore, to test the reproducibility, a repeat measurement of PWV was obtained in one randomly selected frequency. Blood pressure (BP) was measured by conventional means at each pacing frequency. PWV appeared fairly reproducible because no significant difference was disclosed between the 2 measurements obtained at the same HR level (P=0.5) and both measurements were strongly correlated (r=0.87,P<0.001). No significant BP variation was observed during pacing. There was a highly significant effect of HR on PWV estimated by a one-way, within-subjects analysis of variance (P=0.01). This study demonstrates that HR is an important factor in the intraindividual variation of PWV in elderly subjects. This raises methodological concern about the measurement of this parameter. Standardizing PWV for HR level seems mandatory if one wants to interpret PWV changes in clinical trials or in the follow-up of patients.
ISSN:0194-911X
出版商:OVID
年代:2002
数据来源: OVID
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