Early-onset ACE inhibition prevented proteinuria and focal glomerular sclerosis in hypertensive fawn-hooded rats, with 100% survival at 72 weeks compared to 21 of 22 untreated rats dying of ESRD.
Does ACE-i prevent or treat chronic renal damage and improve survival in spontaneously hypertensive fawn-hooded rats?
Early initiation of ACE inhibition is highly effective in preventing renal damage and mortality in a hypertensive rat model, whereas delayed or temporary treatment is insufficient to halt disease progression.
The spontaneously hypertensive fawn-hooded rat (FHH) develops accelerated albuminuria and focal glomerular sclerosis (FGS), leading to ESRD and shortening of lifespan. The FHH is characterized by moderate systemic hypertension, a relatively low afferent to efferent arteriolar resistance ratio, and glomerular hypertension. The FHH study presented here was designed to examine the efficacy of early-onset, late-onset, or early-temporary angiotensin I-converting enzyme inhibition (ACE-i) in ameliorating long-term hypertension and FGS, and improving survival, as well as to relate its protective efficacy to preexistent FGS and to reduction of glomerular pressure (PGC) Untreated rats developed hypertension and high PGC, and all (N = 22) except one died of ESRD within the 72-wk follow-up period. Early-onset (at 7 wk of age) ACE-i prevented development of systemic and glomerular hypertension, and it largely prevented proteinuria and FGS; all rats survived throughout the follow-up period. Rats treated with late-onset (22 wk) ACE-i were hypertensive and proteinuric at the start of ACE-i, and they showed beginning FGS. ACE-i corrected the hypertension, albuminuria, and PGC but could not fully prevent some hypertension, albuminuria, and FGS at the later stage. Early-temporary (7 to 22 wk) ACE-i adequately controlled blood pressure and development of FGS during therapy, but after withdrawal of ACE-i, systemic and glomerular hypertension developed as in untreated animals. This regimen postponed but did not control FGS development and early mortality. The results of this study indicate that: (1) early-onset ACE-i very effectively protects against development of renal damage in the FHH; (2) this protection is associated with normalization of the elevated glomerular capillary pressure; (3) ACE-i cannot completely prevent further development of previously established FGS, despite lowering glomerular capillary pressure; (4) early-temporary ACE-i has no long-term controlling effect on arterial and glomerular pressure, and it cannot control development of FGS.
Verseput et al. (Sat,) conducted a other in Hypertension and chronic renal damage. Angiotensin I-converting enzyme inhibition (ACE-i) vs. Untreated was evaluated on Survival and development of focal glomerular sclerosis. Early-onset ACE inhibition prevented proteinuria and focal glomerular sclerosis in hypertensive fawn-hooded rats, with 100% survival at 72 weeks compared to 21 of 22 untreated rats dying of ESRD.
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