Endothelin-1 is elevated in monocrotaline pulmonary hypertension

被引:82
作者
Frasch, HF [1 ]
Marshall, C [1 ]
Marshall, BE [1 ]
机构
[1] Hosp Univ Penn, Ctr Anesthesia Res, Philadelphia, PA 19104 USA
来源
AMERICAN JOURNAL OF PHYSIOLOGY-LUNG CELLULAR AND MOLECULAR PHYSIOLOGY | 1999年 / 276卷 / 02期
关键词
pulmonary circulation; pulmonary vascular resistance; endothelial function; nitric oxide;
D O I
10.1152/ajplung.1999.276.2.L304
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
These studies document striking pulmonary vasoconstrictor response to nitric oxide synthase (NOS) inhibition in monocrotaline (MCT) pulmonary hypertension in rats. This constriction is caused by elevated endothelin (ET)-1 production acting on ETA receptors. Isolated, red blood cell plus buffer-perfused lungs from rats were studied 3 wk after MCT (60 mg/kg) or saline injection. MOT-injected rats developed pulmonary hypertension, right ventricular hypertrophy, and heightened pulmonary vasoconstriction to ANG II and the NOS inhibitor N-G-monomethyl-L-arginine (L-NMMA). In MCT-injected lungs, the magnitude of the pulmonary presser response to NOS inhibition correlated strongly with the extent of pulmonary hypertension. Pretreatment of isolated MCT-injected lungs with combined ETA (BQ-123) plus ETB (BQ-788) antagonists or ETA antagonist alone prevented the L-NMMA-induced constriction. Addition of ETA antagonist reversed established L-NMMA-induced constriction; ETB antagonist did not. ET-1 concentrations were elevated in MCT-injected lung perfusate compared with sham-injected lung perfusate, but ET-1 levels did not differ before and after NOS inhibition. NOS inhibition enhanced hypoxic pulmonary vasoconstriction in both sham- and MCT-injected lungs, but the enhancement was greater in MCT-injected lungs. Results suggest that in MCT pulmonary hypertension, elevated endogenous ET-1 production acting through ETA receptors causes pulmonary vasoconstriction that is normally masked by endogenous NO production.
引用
收藏
页码:L304 / L310
页数:7
相关论文
共 30 条
[1]  
BARER G, 1993, J PHYSIOL-LONDON, V463, P1
[2]   NORMOBARIC HYPOXIA STIMULATES ENDOTHELIN-1 GENE-EXPRESSION IN THE RAT [J].
ELTON, TS ;
OPARIL, S ;
TAYLOR, GR ;
HICKS, PH ;
YANG, RH ;
JIN, HK ;
CHEN, YF .
AMERICAN JOURNAL OF PHYSIOLOGY, 1992, 263 (06) :R1260-R1264
[3]   CLEARANCE OF CIRCULATING ENDOTHELIN-1 BY ET(B) RECEPTORS IN RATS [J].
FUKURODA, T ;
FUJIKAWA, T ;
OZAKI, S ;
ISHIKAWA, K ;
YANO, M ;
NISHIKIBE, M .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1994, 199 (03) :1461-1465
[4]   EXPRESSION OF ENDOTHELIN-1 IN THE LUNGS OF PATIENTS WITH PULMONARY-HYPERTENSION [J].
GIAID, A ;
YANAGISAWA, M ;
LANGLEBEN, D ;
MICHEL, RP ;
LEVY, R ;
SHENNIB, H ;
KIMURA, S ;
MASAKI, T ;
DUGUID, WP ;
STEWART, DJ .
NEW ENGLAND JOURNAL OF MEDICINE, 1993, 328 (24) :1732-1739
[5]  
HASSOUN PM, 1992, P SOC EXP BIOL MED, V199, P165
[6]   ENDOTHELIN IS A POTENT MITOGEN FOR RAT VASCULAR SMOOTH-MUSCLE CELLS [J].
HIRATA, Y ;
TAKAGI, Y ;
FUKUDA, Y ;
MARUMO, F .
ATHEROSCLEROSIS, 1989, 78 (2-3) :225-228
[7]   INCREASED ENDOTHELIUM-DERIVED NO IN HYPERTENSIVE PULMONARY CIRCULATION OF CHRONICALLY HYPOXIC RATS [J].
ISAACSON, TC ;
HAMPL, V ;
WEIR, EK ;
NELSON, DP ;
ARCHER, SL .
JOURNAL OF APPLIED PHYSIOLOGY, 1994, 76 (02) :933-940
[8]   NITRIC-OXIDE SYNTHASE IN HUMAN AND RAT LUNG - IMMUNOCYTOCHEMICAL AND HISTOCHEMICAL-LOCALIZATION [J].
KOBZIK, L ;
BREDT, DS ;
LOWENSTEIN, CJ ;
DRAZEN, J ;
GASTON, B ;
SUGARBAKER, D ;
STAMLER, JS .
AMERICAN JOURNAL OF RESPIRATORY CELL AND MOLECULAR BIOLOGY, 1993, 9 (04) :371-377
[9]   Chronic hypoxia upregulates endothelial and inducible NO synthase gene and protein expression in rat lung [J].
LeCras, TD ;
Xue, C ;
Rengasamy, A ;
Johns, RA .
AMERICAN JOURNAL OF PHYSIOLOGY-LUNG CELLULAR AND MOLECULAR PHYSIOLOGY, 1996, 270 (01) :L164-L170
[10]   ENHANCED ENDOTHELIN-1 AND ENDOTHELIN RECEPTOR GENE-EXPRESSION IN CHRONIC HYPOXIA [J].
LI, HB ;
CHEN, SJ ;
CHEN, YF ;
MENG, QC ;
DURAND, J ;
OPARIL, S ;
ELTON, TS .
JOURNAL OF APPLIED PHYSIOLOGY, 1994, 77 (03) :1451-1459
123