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101. Sustained influence of the renal nerves to attenuate sodium retention in angiotensin hypertension

Author

LOHMEIER, THOMAS E., LOHMEIER, JUSTIN R., RECKELHOFF, JANE F., and HILDEBRANDT, DREW A.

Subjects
Kidneys -- Physiological aspects, Sodium in the body -- Physiological aspects, Angiotensin -- Physiological aspects, Hypertension -- Physiological aspects, Nervous system, Sympathetic -- Physiological aspects, Biological sciences
Abstract

Recent studies indicate that baroreflex suppression of renal sympathetic nerve activity is sustained for up to 5 days of ANG II infusion; however, steady-state conditions are not associated with ANG II hypertension of this short duration. Thus the major goal of this study was to determine whether neurally induced increments in renal excretory function during chronic intravenous infusion of ANG II are sustained under more chronic conditions when hypertension is stable and sodium balance is achieved. Experiments were conducted in five conscious dogs subjected to unilateral renal denervation and surgical division of the urinary bladder into hemibladders to allow separate 24-h urine collection from denervated (Den) and innervated (Inn) kidneys. ANG II was infused after control measurements for 10 days at a rate of 5 [ng [multiplied by] [kg.sup.-1] [multiplied by] [min.sup.-1]]. Twenty-four-hour control values for mean arterial pressure (MAP) and the ratio for urinary sodium excretion from Den and Inn kidneys (Den/Inn) were 92 [+ or -] 4 mmHg and 0.99 [+ or -] 0.05, respectively. On days 8-10 of ANG II infusion, MAP was stable (+30 [+ or -] 3 mmHg) and sodium balance was achieved. Whereas equal amounts of sodium were excreted from the kidneys during the control period, throughout ANG II infusion there was a greater rate of sodium excretion from Inn vs. Den kidneys (day 10 Den/Inn sodium = 0.56 [+ or -] 0.05), indicating chronic suppression of renal sympathetic nerve activity. The greater rate of sodium excretion in Inn vs. Den kidneys during renal sympathoinhibition also revealed a latent impairment in sodium excretion from Den kidneys. Although the Den/Inn for sodium and the major metabolites of nitric oxide (NO) decreased in parallel during ANG II hypertension, the Den/Inn for cGMP, a second messenger of NO, remained at control levels throughout this study. This disparity fails to support the notion that a deficiency in NO production and action in Den kidneys accounts for the impaired sodium excretion. Most importantly, these results support the contention that baroreflex suppression of renal sympathetic nerve activity is sustained during chronic ANG II hypertension, a response that may play an important role in attenuating the rise in arterial pressure. baroreflexes; sympathetic nervous system; kidneys; nitric oxide

Published
2001

110. Report of the National Heart, Lung, and Blood Institute Working Group on Sex Differences Research in Cardiovascular Disease

Author

Maric-Bilkan, Christine, primary, Arnold, Arthur P., additional, Taylor, Doris A., additional, Dwinell, Melinda, additional, Howlett, Susan E., additional, Wenger, Nanette, additional, Reckelhoff, Jane F., additional, Sandberg, Kathryn, additional, Churchill, Gary, additional, Levin, Ellis, additional, and Lundberg, Martha S., additional

Published
2016
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117. Sex Differences in the Cardiovascular Consequences of Diabetes Mellitus

Author

Regensteiner, Judith G., primary, Golden, Sherita, additional, Huebschmann, Amy G., additional, Barrett-Connor, Elizabeth, additional, Chang, Alice Y., additional, Chyun, Deborah, additional, Fox, Caroline S., additional, Kim, Catherine, additional, Mehta, Nehal, additional, Reckelhoff, Jane F., additional, Reusch, Jane E.B., additional, Rexrode, Kathryn M., additional, Sumner, Anne E., additional, Welty, Francine K., additional, Wenger, Nanette K., additional, and Anton, Blair, additional

Published
2015
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119. Androgens and Blood Pressure Control

Author

Reckelhoff, Jane F.

Abstract

The role that androgens play in mediating elevated blood pressure is unclear. Low levels of androgens in men and increased levels of androgens in women, as occurs with polycystic ovary syndrome (PCOS), are both associated with increased risk for cardiovascular disease and elevated blood pressure. We have used animal models to evaluate the potential mechanisms by which men and women have differential responses to androgens that affect regulation of blood pressure and the implications these may have for the health of men and women.

Published
2019
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126. Roles for the sympathetic nervous system, renal nerves, and CNS melanocortin-4 receptor in the elevated blood pressure in hyperandrogenemic female rats

Author

Maranon, Rodrigo, primary, Lima, Roberta, additional, Spradley, Frank T., additional, do Carmo, Jussara M., additional, Zhang, Howei, additional, Smith, Andrew D., additional, Bui, Elizabeth, additional, Thomas, R. Lucas, additional, Moulana, Mohadetheh, additional, Hall, John E., additional, Granger, Joey P., additional, and Reckelhoff, Jane F., additional

Published
2015
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128. Cardiometabolic Features of Polycystic Ovary Syndrome: Role of Androgens.

Author

Cardozo, Licy L. Yanes, Romero, Damian G., and Reckelhoff, Jane F.

Subjects
POLYCYSTIC ovary syndrome, ENDOCRINE diseases, METABOLIC disorders, ANDROGENS, HEART disease risk factors, DISEASE risk factors
Abstract

Polycystic ovary syndrome (PCOS) is the most common endocrine disorder that affects reproductive-age women. Hyperandrogenemia is present in a significant fraction (~80%) of women with PCOS. Increased prevalence of cardiometabolic risk factors is frequently observed in PCOS women. The present review aims to highlight the key role of androgens in mediating the negative cardiometabolic profile observed in PCOS women. [ABSTRACT FROM AUTHOR]

Published
2017
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144. Low-dose testosterone protects against renal ischemia-reperfusion injury by increasing renal IL-10-to-TNF-α ratio and attenuating T-cell infiltration.

Author

Patil, Chetan N., Wallace, Kedra, LaMarca, Babbette D., Moulana, Mohadetheh, Lopez-Ruiz, Arnaldo, Soljancic, Andrea, Juncos, Luis A., Grande, Joseph P., and Reckelhoff, Jane F.

Abstract

Renal ischemia-reperfusion (I/R) in male rats causes reductions in plasma testosterone, and infusion of testosterone 3 h postreperfusion is protective. We tested the hypotheses that acute high doses of testosterone promote renal injury after I/R, and that acute low-dose testosterone is protective by the following: 1) increasing renal IL-10 and reducing TNF-α; 2) its effects on nitric oxide; and 3) reducing intrarenal T-cell infiltration. Rats were subjected to renal I/R, followed by intravenous infusion of vehicle or testosterone (20, 50, or 100 μg/kg) 3 h postreperfusion. Low-dose testosterone (20 μg/kg) reduced plasma creatinine, increased nitrate/nitrite excretion, increased intrarenal IL-10, and reduced intrarenal TNF-α, whereas 50 μg/kg testosterone failed to reduce plasma creatinine, increased IL-10, but failed to reduce TNF-α. A higher dose of testosterone (100 mg/kg) not only failed to reduce plasma creatinine, but significantly increased both IL-10 and TNF-α compared with other groups. Low-dose nitro-l-arginine methyl ester (1 mg·kg-1·day-1), given 2 days before I/R, prevented low-dose testosterone (20 μg/kg) from protecting against I/R injury, and was associated with lack of increase in intrarenal IL-10. Intrarenal CD4+ and CD8+ T cells were significantly increased with I/R, but were attenuated with low-dose testosterone, as were effector T helper 17 cells. The present studies suggest that acute, low-dose testosterone is protective against I/R AKI in males due to its effects on inflammation by reducing renal T-cell infiltration and by shifting the balance to favor anti-inflammatory cytokine production rather than proinflammatory cytokines. [ABSTRACT FROM AUTHOR]

Published
2016
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145. 20-HETE and CYP4A2 ω-hydroxylase contribute to the elevated blood pressure in hyperandrogenemic female rats.

Author

Dalmasso, Carolina, Maranon, Rodrigo, Patil, Chetan, Moulana, Mohadetheh, Romero, Damian G., and Reckelhoff, Jane F.

Subjects
HEMODYNAMICS, BLOOD pressure
Abstract

In male rats, androgen supplements increase 20-hydroxyeicosatetraenoic acid (20-HETE) via cytochrome P-450 (CYP)4A ω-hydroxylase and cause an increase in blood pressure (BP). In the present study, we determined the roles of 20-HETE and CYP4A2 on the elevated BP in hyperandrogenemic female rats. Chronic dihydrotestosterone (DHT) increased mean arterial pressure (MAP) in female Sprague-Dawley rats (96 ± 2 vs. 108 ± 2 mmHg, P < 0.05) and was associated with increased renal microvascular CYP4A2 mRNA expression (15-fold), endogenous renal 20-HETE (5-fold), and ω-hydroxylase activity (3-fold). Chronic DHT also increased MAP in low salt-fed Dahl salt-resistant female rats (81 ± 4 vs. 95 ± 1 mmHg, P < 0.05) but had no effect on MAP in Dahl salt-sensitive female rats (154 ± 3 vs. 153 ± 3 mmHg), which are known to be 20-HETE deficient. To test the role of CYP4A2, female CYP4A2−/− and SS.5Bn (wild type) rats were treated with DHT. DHT increased MAP in SS.5Bn female rats (104 ± 1 vs. 128 ± 1 mmHg, P < 0.05) but had no effect in CYP4A2−/− female rats (118 ± 1 vs. 120 ± 1 mmHg). Renal microvascular 20-HETE was reduced in control CYP4A2−/− female rats and was increased with DHT in SS.5Bn female rats (6-fold) but not CYP4A2−/− female rats. ω-Hydroxylase activity was 40% lower in control CYP4A2−/− female rats than in SS.5Bn female rats, and DHT decreased ω-hydroxylase activity in SS.5Bn female rats (by 50%) but significantly increased ω-hydroxylase activity in CYP4A2−/− female rats (3-fold). These data suggest that 20-HETE via CYP4A2 contributes to the elevation in BP in hyperandrogenemic female rats. The data also suggest that 20-HETE synthesis inhibition may be effective in treating the elevated BP in women with hyperandrogenemia, such as women with polycystic ovary syndrome. [ABSTRACT FROM AUTHOR]

Published
2016
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