AFLUID July 46/1
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چکیده
Ichihara, Atsuhiro, and L. Gabriel Navar. Neuronal NOS contributes to biphasic autoregulatory response during enhanced TGF activity. Am. J. Physiol. 277 (Renal Physiol. 46): F113–F120, 1999.—To assess the afferent arteriolar autoregulatory response during increased activity of the tubuloglomerular feedback (TGF) mechanism and to delineate the contribution of neuronal nitric oxide synthase (nNOS) to this response, afferent arteriolar diameter responses to changes in renal perfusion pressure (RPP) were monitored in vitro using the blood-perfused rat juxtamedullary nephron preparation. At RPP of 100 mmHg, basal afferent arteriolar diameter averaged 21.1 6 1.4 μm (n 5 9). The initial and sustained constrictor responses of afferent arterioles to a 60-mmHg increase in RPP averaged 14.8 6 1.4% and 13.3 6 1.3%, respectively. Acetazolamide treatment, which enhances TGF responsiveness by increasing distal nephron volume delivery, significantly decreased basal afferent arteriolar diameter by 8.2 6 0.5% and enhanced the initial response (25.5 6 2.3%) to a 60-mmHg increase in RPP but did not alter the sustained response (14.3 6 1.5%). In another series of experiments, nNOS inhibition with 10 μM S-methyl-Lthiocitrulline (L-SMTC) significantly decreased afferent arteriolar diameter from 20.3 6 1.3 to 18.3 6 1.1 μm (n 5 7) and enhanced both the initial (34.4 6 3.5%) and sustained constrictor responses (27.6 6 2.9%) to a 60-mmHg increase in RPP. Treatment with acetazolamide further enhanced both initial (56.4 6 3.0%) and sustained responses (54.6 6 2.7%). Interruption of distal delivery by transection of the loops of Henle prevented the enhanced responses to increases in RPP elicited with either acetazolamide or L-SMTC. These results indicate that nNOS contributes to the counteracting resetting process of biphasic afferent arteriolar constrictor responses to increases in RPP through a TGF-dependent mechanism.
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AFLUID July 46/1
DOUGLAS N. HENRY,1,2 JULIA V. BUSIK,1 FRANK C. BROSIUS III,3 AND CHARLES W. HEILIG4 1Department of Physiology, 2Department of Pediatrics and Human Development, Division of Pediatric Endocrinology, College of Human Medicine, Michigan State University, East Lansing 48824-1101; 3Department of Medicine, Division of Nephrology, University of Michigan Medical School and Ann Arbor Veterans Affairs Hos...
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متن کاملAFLUID November 46/5
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متن کاملAFLUID October 46/4
Hediger, Matthias A. Glutamate transporters in kidney and brain. Am. J. Physiol. 277 (Renal Physiol. 46): F487–F492, 1999.—Glutamate transporters play important roles in the termination of excitatory neurotransmission and in providing cells with glutamate for metabolic purposes. In the kidney, glutamate transporters are involved in reabsorption of filtered acidic amino acids, regulation of ammo...
متن کاملAFLUID July 46/1
Thomson, R. Brent, and Peter S. Aronson. Immunolocalization of Ksp-cadherin in the adult and developing rabbit kidney. Am. J. Physiol. 277 (Renal Physiol. 46): F146–F156, 1999.—The potential for Ksp-cadherin involvement in either the development or maintenance of the metanephric kidney was assessed by immunocytochemical localization of a monoclonal antibody directed against the rabbit isoform o...
متن کاملAFLUID July 46/1
Conrad, Kirk P., Laurie J. Kerchner, and Monique D. Mosher. Plasma and 24-h NOx and cGMP during normal pregnancy and preeclampsia in women on a reduced NOx diet. Am. J. Physiol. 277 (Renal Physiol. 46): F48–F57, 1999.—We tested the hypothesis that nitric oxide (NO) biosynthesis increases during normal human pregnancy and decreases in preeclampsia. The major metabolites of NO, nitrate and nitrit...
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