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Kidney failure and ARBs

INTRDUCTION
Diabetic nephropathy is the leading cause of end-stage
kidney disease. Slowing down the RAS (renin-angiotensin
system) slows the worsening of kidney disease in patients
with type one diabetes but we don't know about typw 2
diabetes patients.
	We studied the role of the ARB Cozaar in
patients with type 2 diabetes and kidney failure.

METHODS
1,513 patients participated. This was a randomized,
double-blind study comparing 50mg to 100mg losartan
daily versus placebo. Patients kept taking their usual
meds (mostly diuretics, calcium channel blockers, nitro,
and beta-blockers). Follow-up was an average of 3.4
years.
	Primary endpoint was doubling of starting
blood creatinine level, end-stage kidney disease, or death.
Secondary endpoints were heart-related complications or
death; proteinuria; and how fast kidney disease got worse.

RESULTS
327 patients in the losartan group suffered the primary end-
point, compared to 359 in the placebo group. Losartan
reduced risk of doubling blood creatinine level and end-
stage kidney disease, but did not affect risk of death.
	Heart-related complications and death risk was
similar in the 2 groups. Risk of first hospitalization for HF
was lower with losartan. Level of proteinuria went down
35% with losartan compared to placebo.

CONCLUSIONS
Losartan gave kidney benefits in patients with type 2
diabetes and nephropathy and was usually well tolerated.

Title:         Effects of losartan on renal and cardiovascular
                 outcomes in patients with type 2 diabetes and
                 nephropathy.
Authors:    Brenner BM, Cooper ME, de Zeeuw D, Keane
                 WF, Mitch WE, Parving HH, Remuzzi G,
                 Snapinn SM, Zhang Z, Shahinfar S.
Source:      N Engl J Med 2001 Sep 20;345(12):861-9
Comment: N Engl J Med. 2001 Sep 20;345(12):910-2
PMID:       11565518
=========================

ACE inhibitors and ARBs increase kidney blood flow, but
the kidneys' glomerular filtration rate does not change.
Both drugs reduce blood pressure, pressure in the kidneys,
and proteinuria. These effects may protect the kidneys.
	Studies show that the kidney-protective effects
of ACE inhibitors and ARBs come from inhibiting
angiotensin 2 and not from inhibiting bradykinin
degradation. Several studies suggest other kidney-protective
effects of ACE inhibitors and ARBs.

Title:       Angiotensin II type-1-receptor antagonists from
               the viewpoint of nephrology.
Authors: Hauser AC, Horl WH.
Source:   Wien Med Wochenschr 2001;151(7-8):160-4
PMID:    11450164
=========================

INTRODUCTION
Blood pressure reduction is the most significant factor in
delaying onset and worsening of kidney disease. Blocking
the RAS (renin-angiotensin system) using ACE inhibitors
slows the worsening of kidney disease. More recently,
ARBs have been used to further protect the kidneys.
	Trials with a variety of ARBs have clearly
shown their anti-proteinuric effectiveness in kidney
disease patients. The effects of ARBs are similar to those
of ACE inhibitors.
	The role of ARBs in high blood pressure
patients with type 2 diabetes is being studied in 3 large
trials:

1) Appropriate Blood Pressure Control in Diabetes-Part 2
    With Valsartan
2) Losartan Renal Protection Study
3) Irbesartan Diabetic Nephropathy Trial

Definite evidence of the long-term protective effects of
ARBs in chronic kidney disease is expected from these
studies.

Title:     Angiotensin II subtype 1 receptor blockers and
              renal function.
Author: Toto R. [robert.toto@utsouthwestern.edu]
Source: Arch Intern Med 2001 Jun 25;161(12):1492-9
PMID:  11427096
=========================

INTRODUCTION
Long-term ACE inhibitor therapy leads to angiotensin
1 accumulation which may "escape" ACE inhibition,
harming patients with chronic kidney disease. We
studied whether adding losartan to maximum ACE
inhibitor therapy (40mg lisinopril daily) blocked more
angiotensin 2 in patients with chronic kidney failure
with high blood pressure.

METHODS
16 patients with chronic kidney failure completed a
crossover, randomized, controlled trial. Each period
was one month, with a 2 week washout between
periods.
	12 patients had diabetic nephropathy and
4 had chronic glomerulonephritis. Average patient age
was 53 years.
	In one period, patients took 40mg lisinopril
daily along with their other blood pressure meds. In the
other period, they took 50mg losartan daily in addition
to their other blood pressure meds.
	We measured walking blood pressure, kidney
function (glomerular filtration rate), and heart output.
Resting blood renin activity, blood aldosterone and urine
protein were also measured in all patients.

RESULTS
Seated blood pressure was 156/88 mmHg. Pulse rate was
77. Cardiac index was 2.9 L/min/m(2). Average 24-hour
protein excretion/gram creatinine did not change.
	Average change in protein excretion that was
due to losartan was +1%. Change in systolic walking
blood pressure due to losartan was 4.6 mmHg and change
in diastolic was 1.5 mmHg. No change was seen in heart
output.
	However, there was an average 14% increase
in glomular filtration rate due to losartan. A fall in blood
renin activity of 32% was also seen. No electrolyte
problems were seen.

CONCLUSIONS
Add-on losartan therapy did not improve proteinuria or
walking blood pressure over one month. However, there
were improvements in glomular filtration rate and a fall
in blood renin level.
	Deciding whether add-on ARBs substantially
help kidney failure patients needs larger and longer trials.

Title:     Add-on angiotensin receptor blockade with
             maximized ACE inhibition.
Author: Agarwal R. [ragarwal@iupui.edu]
Source: Kidney Int 2001 Jun;59(6):2282-9
PMID: 11380832
=========================

INTRODUCTION
We studied the effect of losartan on kidney function in
non-diabetic patients with chronic kidney failure. This
was an open, prospective, follow-up study of one year.

METHODS
29 high blood pressure patients (14 females and 15
males with an average age of 63 years) with non-diabetic
chronic kidney failure from several causes participated.
They took 50 mg losartan daily plus any other drugs
they needed. Follow up was 13 months.
	18 patients were taking ACE inhibitors plus
other high blood pressure drugs at study start. Patients
had been followed for almost 4 years previously.
	Worsening of kidney failure was measured
as the slope of the reciprocal of blood creatinine level vs
time in months.

RESULTS		Study start	After one year with losartan

Blood pressure	149/90	142/84 mmHg
Creatinine clearance	29	29 ml/min
Protein excretion	1.7 g/24 h	1.2 g/24 h
Blood creatinine	3.18	3.49 mg/ml
Disease progression	-0.0039	-0.0012 mg/month

CONCLUSIONS
Worsening of kidney function in patients with non-
diabetic chronic kidney failure is slowed down after a
year of losartan treatment. Our results suggest that
ARBs offer kidney protection in this patient subset.
These results need to be confirmed in controlled trials.

Title:       Effect of angiotensin II receptor blockade on
               renal disease progression in patients with
               non-diabetic chronic renal failure.
Authors: Mora-Macia J, Cases A, Calero F, Barcelo P.
Source:   Nephrol Dial Transplant 2001;16 Suppl 1:82-4
PMID:   11369829