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1. |
Council Honorees and the Nobel Prize Our Continued Anniversary Celebration |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 161-161
Edward D. Frohlich,
L. Gabriel Navar,
Richard N. Re,
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ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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2. |
Harriet Pearson Dustan |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 162-163
Edward D. Frohlich,
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ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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3. |
Kallikrein Gene Delivery Inhibits Vascular Smooth Muscle Cell Growth and Neointima Formation in the Rat Artery After Balloon Angioplasty |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 164-170
Hideyuki Murakami,
Katsutoshi Yayama,
Robert Q. Miao,
Cindy Wang,
Lee Chao,
Julie Chao,
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摘要:
Tissue kallikrein cleaves kininogen substrate to produce vasoactive kinin peptides that have been implicated in the proliferation of vascular smooth muscle cells (VSMCs). To explore potential roles of the kallikrein-kinin system in vascular biology, we evaluated the effects of adenovirus-mediated human kallikrein gene delivery on the growth of primary cultured VSMCs and in balloon-injured rat artery in vivo. Kallikrein gene transfer into cultured rat VSMCs resulted in time-dependent secretion of recombinant human tissue kallikrein and inhibition of cell proliferation. Balloon angioplasty reduced endogenous rat tissue kallikrein mRNA and protein levels at the injured site. In rats that received adenovirus-mediated human kallikrein gene delivery, we observed a 39% reduction in intima/media ratio at the injured vessel after delivery compared with that of rats that received control virus (n=8, P<0.01). Icatibant, a specific bradykinin B2receptor antagonist, blocked the protective effect and reversed the intima/media ratio to that of the control rats (n=5, P<0.01). After gene delivery, human kallikrein mRNA was identified at the injured vessel and a 3-fold increase occurred in kininogenase activity. cAMP and cGMP levels in balloon-injured aorta increased significantly at 4, 7, and 14 days after kallikrein gene delivery, but icatibant abolished the increase. These results provide new insights into the role of the vascular kallikrein-kinin system and have significant implications for gene therapy to treat restenosis or atherosclerosis. (Hypertension. 1999;34:164-170.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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4. |
Angiotensin-Converting Enzyme Inhibition Modifies Angiotensin but Not Kinin Peptide Levels in Human Atrial Tissue |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 171-175
Duncan J. Campbell,
Ann-Maree Duncan,
Athena Kladis,
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摘要:
Angiotensin-converting enzyme (ACE) converts angiotensin I (Ang I) to angiotensin II (Ang II) and metabolizes bradykinin and kallidin peptides. Decreased Ang II levels and increased kinin peptide levels are implicated in the mediation of the therapeutic effects of ACE inhibition. However, alternative non-ACE pathways of Ang II formation have been proposed to predominate in human heart. We investigated the effects of ACE inhibition on cardiac tissue levels of angiotensin and kinin peptides. High-performance liquid chromatography-based radioimmunoassays were used to measure angiotensin peptides and hydroxylated and nonhydroxylated bradykinin and kallidin peptides in right atrial appendages of subjects who had been prepared for cardiopulmonary bypass. Peptide levels in subjects who received ACE inhibitor therapy were compared with those who did not receive ACE inhibitor therapy. ACE inhibition reduced Ang II levels, which was associated with an 80% reduction in the Ang II/Ang I ratio. ACE inhibition did not modify either bradykinin or kallidin peptide levels or the bradykinin-(1-7)/bradykinin-(1-9) ratio. The 80% reduction in the Ang II/Ang I ratio by ACE inhibition indicated a primary role for ACE in the conversion of Ang I to Ang II in atrial tissue. These data support a role for reduced Ang II levels but do not support a role for increased kinin peptide levels in mediating the direct cardiac effects of ACE inhibition. (Hypertension. 1999;34:171-175.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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5. |
Early Onset Salt-Sensitive Hypertension in Bradykinin B2Receptor Null Mice |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 176-180
Ludek Cervenka,
Lisa M. Harrison-Bernard,
Susana Dipp,
Ginny Primrose,
John D. Imig,
Samir S. El-Dahr,
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摘要:
Kinins have been implicated in the hemodynamic adaptation to postnatal life. The present study examined the impact of bradykinin B2receptor (B2R) gene disruption on the postnatal changes in blood pressure (BP) and the susceptibility to early onset salt-sensitive hypertension in mice. B2R null (-/-) and wild-type (+/+) mice were fed normal (NS, 1% NaCl) or high (HS, 5% NaCl) salt diets during pregnancy. After birth, the pups remained with their mothers until they were weaned and were subsequently continued on the respective maternal salt intake until 4 months of age. The age-related changes at 3 and 4 months in tail-cuff BP and anesthetized mean arterial pressure at 4 months were not different in NS/B2R-/-and NS/B2R+/+mice. However, there was a mild increase in BP in NS/B2R-/-at 2 months versus NS/B2R+/+. In contrast, HS/B2R-/-mice manifested early onset and persistent elevations of tail-cuff BP (P<0.05) at 2, 3, and 4 months versus other groups. MAP was also higher in HS/B2R-/-than HS/B2R+/+, NS/B2R-/-, and NS/B2R+/+(91 +/- 3 versus 75 +/- 5, 74 +/- 2, and 70 +/- 2 mm Hg, respectively; P<0.05). Kidney renin and angiotensin type 1 receptor mRNA levels were not different. Additional studies showed that a delay in the initiation of HS until after birth was accompanied by later development of hypertension, although postnatal discontinuation of HS resulted in a gradual return of BP to normal values by 4 months of age. The results demonstrate that (1) kinins protect the developing animal from salt-sensitive hypertension, (2) lack of B2R from early development does not alter the maturation of BP under conditions of normal sodium intake, and (3) exposure to a HS diet during fetal life is not sufficient in itself to induce long-term hypertension in either wild-type or B2R null mice. (Hypertension. 1999;34:176-180.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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6. |
Effects of Potassium on Blood Pressure in Salt-Sensitive and Salt-Resistant Black Adolescents |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 181-186
Dawn K. Wilson,
Domenic A. Sica,
Sydney B. Miller,
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摘要:
or=to5 mm Hg from the low to high sodium diet. Sixteen salt-sensitive and 42 salt-resistant subjects were then randomly assigned to either a 3-week high potassium diet (80 mmol/24 h) or usual diet control group. Urinary potassium excretion significantly increased in the treatment group (35 +/- 7 to 57 +/- 21 mmol/24 h). At baseline, a significantly greater percentage of salt-sensitive (44%) compared with salt-resistant (7%) subjects were nondippers on the basis of diastolic blood pressure classifications (P<0.04). After the dietary intervention, all of the salt-sensitive subjects in the high potassium group achieved dipper status as a result of a drop in nocturnal diastolic blood pressure (daytime, 69 versus 67 mm Hg; nighttime, 69 versus 57 mm Hg). No significant group differences in cardiovascular reactivity were observed. These results suggest that a positive relationship between dietary potassium intake and blood pressure modulation can still exist even when daytime blood pressure is unchanged by a high potassium diet. (Hypertension. 1999;34:181-186.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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7. |
Genetic Isolation of a Chromosome 1 Region Affecting Susceptibility to Hypertension-Induced Renal Damage in the Spontaneously Hypertensive Rat |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 187-191
Elizabeth St. Lezin,
Karen A. Griffin,
Maria Picken,
Monique C. Churchill,
Paul C. Churchill,
Theodore W. Kurtz,
Weizhong Liu,
Ning Wang,
Vladimir Kren,
Vaclav Zidek,
Michal Pravenec,
Anil K. Bidani,
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摘要:
Linkage studies in the fawn-hooded hypertensive rat have suggested that genes influencing susceptibility to hypertension-associated renal failure may exist on rat chromosome 1q. To investigate this possibility in a widely used model of hypertension, the spontaneously hypertensive rat (SHR), we compared susceptibility to hypertension-induced renal damage between an SHR progenitor strain and an SHR congenic strain that is genetically identical except for a defined region of chromosome 1q. Backcross breeding with selection for the markers D1Mit3 and Igf2 on chromosome 1 was used to create the congenic strain (designated SHR.BN-D1Mit3/Igf2) that carries a 22 cM segment of chromosome 1 transferred from the normotensive Brown Norway rat onto the SHR background. Systolic blood pressure (by radiotelemetry) and urine protein excretion were measured in the SHR progenitor and congenic strains before and after the induction of accelerated hypertension by administration of DOCA-salt. At the same level of DOCA-salt hypertension, the SHR.BN-D1Mit3/Igf2 congenic strain showed significantly greater proteinuria and histologically assessed renal vascular and glomerular injury than the SHR progenitor strain. These findings demonstrate that a gene or genes that influence susceptibility to hypertension-induced renal damage have been trapped in the differential chromosome segment of the SHR.BN-D1Mit3/Igf2 congenic strain. This congenic strain represents an important new model for the fine mapping of gene(s) on chromosome 1 that affect susceptibility to hypertension-induced renal injury in the rat. (Hypertension. 1999;34:187-191.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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8. |
Inhibition of the p53 Tumor Suppressor Gene Results in Growth of Human Aortic Vascular Smooth Muscle CellsPotential Role of p53 in Regulation of Vascular Smooth Muscle Cell Growth |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 192-200
Motokuni Aoki,
Ryuichi Morishita,
Hidetsugu Matsushita,
Shin-ichiro Hayashi,
Hironori Nakagami,
Kei Yamamoto,
Atsushi Moriguchi,
Yasufumi Kaneda,
Jitsuo Higaki,
Toshio Ogihara,
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摘要:
Loss of activity of the p53 tumor suppressor gene product has been postulated in the pathogenesis of human restenosis. Although the antioncogenes p53 and retinoblastoma (Rb) susceptibility gene have been reported to play a pivotal role in cell cycle progression in various cells, the role of p53 and Rb in the growth of human vascular smooth muscle cells (VSMC) has not yet been clarified. We used antisense strategy against p53 and Rb genes by the viral envelope-liposomal method. Transfection of antisense p53 oligodeoxynucleotides (ODN) alone resulted in an increase in DNA synthesis compared with control (P<0.01). Similarly, transfection of antisense Rb ODN alone resulted in a higher DNA synthesis rate than control (P<0.01). Moreover, increase in VSMC number was only induced by transfection of antisense p53 ODN alone or cotransfection of p53/Rb ODN (P<0.01), whereas a single transfection of antisense Rb ODN had little effect on cell number. Therefore, we hypothesized that this discrepancy is due to the induction of apoptosis mediated by p53. Interestingly, apoptotic cells were markedly increased in VSMC transfected with antisense Rb ODN alone, accompanied by the induction of p53 protein. The number of apoptotic cells was attenuated by cotransfection of antisense p53 ODN (P<0.01). We finally examined the molecular mechanisms of apoptosis induced by the absence of Rb. In VSMC transfected with antisense Rb ODN, bax, a promoter of apoptosis, was significantly increased in VSMC transfected with antisense Rb ODN (P<0.01), whereas bcl-2 and Fas did not play a pivotal role in the induction of apoptosis. Overall, these data first demonstrated that the antioncogenes p53 and Rb negatively regulated the cell cycle in VSMC, suggesting that the modulation of their activity may mediate VSMC growth such as that in restenosis and atherosclerosis. The presence of p53 plays a pivotal role in the regulation of apoptosis in human VSMC growth, probably through the bax pathway. These results provide evidence that p53 is a functional link between cell growth and apoptosis in VSMC. (Hypertension. 1999;34:192-200.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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9. |
Arterial Stiffness and the Development of Hypertension The ARIC Study |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 201-206
Duanping Liao,
Donna K. Arnett,
Herman A. Tyroler,
Ward A. Riley,
Lloyd E. Chambless,
Moyses Szklo,
Gerardo Heiss,
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摘要:
or=to95 mm Hg, or the use of antihypertensive medication at a follow-up examination conducted every 3 years. The age-, ethnicity-, center-, gender-, education-, smoking-, heart rate-, and obesity-adjusted means (SE) of baseline adjusted arterial diameter change, Peterson's elastic modulus, Young's elastic modulus, and beta stiffness index were 397 (5), 148 (2.0), 787 (12.7), and 11.43 (0.16), respectively, in persons who developed hypertension during follow-up, in contrast to 407 (1), 124 (0.6), 681 (3.7), and 10.34 (0.05), respectively, for persons who did not. The similarly adjusted cumulative incident rates of hypertension from the highest to the lowest quartiles of arterial elasticity were 6.7%, 8.0%, 7.3%, and 9.6%, respectively, when measured by adjusted arterial diameter change (P<0.01). One standard deviation decrease in arterial elasticity was associated with 15% greater risk of hypertension, independent of established risk factors for hypertension and the level of baseline blood pressure. These results suggest that lower arterial elasticity is related to the development of hypertension. (Hypertension. 1999;34:201-206.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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10. |
Effects of Aging and Antihypertensive Treatment on Aortic Internal Diameter in Spontaneously Hypertensive Rats |
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Hypertension,
Volume 34,
Issue 2,
1999,
Page 207-211
Philippe Giummelly,
Isabelle Lartaud-Idjouadiene,
Valerie Marque,
Nathalie Niederhoffer,
Jean-Marc Chillon,
Christine Capdeville-Atkinson,
Jeffrey Atkinson,
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摘要:
The effect of antihypertensive treatment on the development of large-artery remodeling in young animals has been widely studied, but reversal of established changes in older hypertensive animals has been largely ignored, although the latter represents a better paradigm for the human condition. We studied the effect of treatment with captopril plus hydrochlorothiazide, from 3 months onward, on geometry and wall stress of the thoracic aorta of adult (9 months, maturation) and old (15 months, senescence) spontaneously hypertensive rats; normotensive Wistar-Kyoto rats were used as controls. At 3 months of age, blood pressure, medial cross-sectional area, and internal diameter were higher in spontaneously hypertensive rats than in Wistar-Kyoto rats. In both strains, medial cross-sectional area and lumen diameter increased during maturation; there was little change with senescence. Changes in blood pressure were minor. Because medial hypertrophy failed to compensate for the wider lumen and higher intraluminal pressure in spontaneously hypertensive rats, medial stress was higher in these rats than in Wistar-Kyoto rats. Captopril plus hydrochlorothiazide rapidly lowered blood pressure and medial cross-sectional area. Despite a marked fall in blood pressure, the internal diameter of the thoracic aorta of treated animals was similar to that of untreated animals after 6 months of treatment and started to fall only after the animals had been treated for 1 year. Thus, under treatment with captopril plus hydrochlorothiazide, medial stress remained elevated, even after very-long-term treatment, because medial cross-sectional area was not adapted to internal diameter. We suggest that some changes in large-artery structure associated with hypertension and aging, such as the increase in diameter, take considerable time to regress after blood pressure is lowered, and this may explain why, despite treatment, wall stress remains elevated. (Hypertension. 1999;34:207-211.)
ISSN:0194-911X
出版商:OVID
年代:1999
数据来源: OVID
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