Based mostly on these observations, we conclude that renovascu lar hypertension markedly accelerates renal illness pro gression in db db mice as characterized by glomerular mesangial matrix expansion, progressive interstitial fibrosis and inflammation, and breakdown on the filtration barrier. This is often in accordance with clinical observations indicating that progression of diabetic nephropathy is accelerated in patients with hypertension. We infused db db mice with angiotensin II for 4 weeks to address a likely part of angiotensin II induced hypertension on renal architecture in db db mice. These mice developed hypertension to levels just like those attained in db RAS mice, however we observed a minimal in crease in mesangial matrix deposition and no evidence of de novo glomerular fibronectin deposition.
Neverthe selleckchem significantly less, db Ang II developed albuminuria similar to that ob served in db RAS mice and also to that reported following angiotensin II infusion to non diabetic mice. Taken together, these observations recommend the professional gressive and bilateral renal injury in db RAS mice is just not mechanistically relevant to elevated angiotensin II amounts alone, although angiotensin II plays a major purpose in de velopment of albuminuria within this model. This come across ing underscores a essential function for activation of your renin angiotensin procedure within the growth of albuminuria and presents a therapeutic rationale for the widespread use of renin angiotensin inhibitors in treatment method of chronic kidney ailment.
We then sought to find out whether hyperfiltration related with unilateral nephrectomy may possibly underlie the progressive renal damage observed inside the contralateral db RAS kidney. Unlike db RAS or db Ang II mice, db UNX did not produce substantial hypertension. Db UNX also didn’t develop greater urine albumin excretion that was observed within the db RAS or selleck db Ang II. Having said that, as shown before, db db mice with unilateral nephrec tomy did create higher glomerular mesangial matrix expansion than age matched db db mice with two child neys, whilst its extent was less than that of db RAS mice. Even though couple of investigators have immediately re ported the extent of interstitial fibrosis on this model, db db mice evaluated at 14 18 weeks submit UNX exhib ited a modest boost in interstitial inflammation, inter stitial volume, and number of tubules showing dilation or atrophy.
While in the recent examine, we find that db UNX mice, in striking contrast to db RAS mice, do not develop significant interstitial fibrosis or tubular at rophy at 4 weeks submit UNX. Hence, glomerular mesangial matrix expansion in db db mice could be attrib uted not less than in aspect to hemodynamic elements associated with hyperfiltration.