Documenti di Didattica
Documenti di Professioni
Documenti di Cultura
Data, Results, and Consequences of Major Trials With Focus on Type 2 Diabetes
Proceedings from a Symposium
ORIGINAL ARTICLE
Raymond O. Estacio, MD
Barrett W. Jeffers, MSC
Nancy Gifford, RN
Robert W. Schrier, MD
RESULTS The mean blood pressure achieved was 132/78 mmHg in the intensive group
and 138/86 mmHg in the moderate control group. During the 5-year follow-up period, no
difference was observed between intensive versus moderate blood pressure control and
those randomized to nisoldipine versus enalapril with regard to the change in creatinine
clearance. After the first year of antihypertensive treatment, creatinine clearance stabilized
in both the intensive and moderate blood pressure control groups in those patients with
baseline normo- or microalbuminuria. In contrast, patients starting with overt albuminuria
demonstrated a steady decline in creatinine clearance of 56 ml min1 1.73 m2 per year
throughout the follow-up period whether they were on intensive or moderate therapy. There
was also no difference between the interventions with regard to individuals progressing
from normoalbuminuria to microalbuminuria (25% intensive therapy vs. 18% moderate
therapy, P = 0.20) or microalbuminuria to overt albuminuria (16% intensive therapy vs.
23% moderate therapy, P = 0.28). Intensive therapy demonstrated a lower overall incidence
of deaths, 5.5 vs. 10.7%, P = 0.037. Over a 5-year follow-up period, there was no difference
between the intensive and moderate groups with regard to the progression of diabetic
retinopathy and neuropathy. In addition, the use of nisoldipine versus enalapril had no
differential effect on diabetic retinopathy and neuropathy.
The 470 patients in the hypertensive cohort of the ABCD Trial, defined as a diastolic blood
pressure >90 mmHg, were randomized to either a moderate (diastolic blood pressure goal
of 8089 mmHg) or intensive (diastolic blood pressure goal of 75 mmHg) blood pressure
reduction goal. The study also evaluated the effects of a long-acting calcium channel
antagonist (nisoldipine) versus an ACE inhibitor (enalapril). The primary end point of the
study was change of creatinine clearance, but the effects of the different blood pressure
levels on retinopathy, neuropathy, and CVD were also addressed. Recently, we reported in
this same cohort that treatment with the ACE inhibitor enalapril was associated with
significantly fewer cardiovascular outcomes (specifically myocardial infarctions) than in
patients treated with the long-acting calcium channel blocker (CCB) nisoldipine (20). The
current article focuses on the effect of moderate (mean 138/86 mmHg) versus intensive
(mean 132/78 mmHg) blood pressure control using either nisoldipine or enalapril in
hypertensive type 2 diabetic patients with nephropathy, retinopathy, and neuropathy
followed for over 5 years.
Design
There were 470 hypertensive type 2 diabetic subjects in the ABCD Trial randomized to
moderate versus intensive antihypertensive treatment (18). Within the moderate (diastolic
blood pressure goal of 8089 mmHg) and intensive (diastolic blood pressure goal of 75
mmHg) treatment groups, patients were further randomized to receive either nisoldipine or
enalapril as the primary antihypertensive medication. The primary objective of the study
was to determine the effect of moderate versus intensive blood pressure control on the
change in creatinine clearance. The ABCD Trial design has been described previously (18).
Participants
Subjects in the ABCD Trial were between the ages of 40 and 74 years at the time of
recruitment and were identified from Diagnosis Related Group, pharmacy, and billing lists
from participating health care systems in the Denver metropolitan area. All patients in the
ABCD Trial were diagnosed with type 2 diabetes according to the criteria based on the
World Health Organization report of 1985 (21). All enrolled hypertensive subjects had a
diastolic blood pressure >90 mmHg and were off all antihypertensive medications at the
randomization visit. Patients were excluded if they had a known allergy to dihydropyridines
or ACE inhibitors, had a myocardial infarction or cerebral vascular accident within the
previous 6 months, had coronary artery bypass surgery within the previous 3 months, had
unstable angina pectoris within the previous 6 months, had Class III or IV New York Heart
Association classification of congestive heart failure, demonstrated an absolute need for
ACE inhibitors or CCBs, received hemo- or peritoneal dialysis, and/or had a serum
creatinine level >3 mg/dl.
At 67 months after the first patient was randomized into the study, the Data Safety
Monitoring Committee (DSMC) observed a significant difference in cardiovascular events
(specifically myocardial infarctions) between study drugs in the hypertensive cohort, which
has been discussed previously (20). Based on this information, the DSMC recommended
switching the nisoldipine-treated patients in the hypertensive group to enalapril treatment.
Diabetic neuropathy
The presence and progression of diabetic neuropathy was assessed according to the criteria
established by Dyck (27). These criteria include neurological symptoms score, neurological
disability score, autonomic nervous system testing with heart rate response to deep
breathing, and quantitative sensory examination performed at baseline and then at year 2
and 5.
Cardiovascular disease
An independent end point committee, which was blinded to the study intervention arms,
reviewed all cardiovascular events. Cardiovascular outcomes were defined as follows: 1)
death due to cardiovascular events (sudden death, progressive heart failure, fatal myocardial
infarction, fatal arrhythmias, cerebral vascular accidents, and ruptured aortic aneurysm), 2)
nonfatal myocardial infarction, 3) nonfatal cerebral vascular accident, 4) heart failure
requiring hospital admission, and 5) pulmonary infarction. The end point committee
reviewed all hospital admissions that appeared to be related to a cardiovascular event.
Statistics
The Statistical Analysis Software (SAS) system was used for all statistical analyses. Two
statistical procedures were used when examining differences in baseline characteristics and
complications between the intensive and moderate therapy groups and between the
nisoldipine and enalapril groups. When the baseline characteristic or complication was
continuous (age, duration of hypertension, duration of diabetes, glycohemoglobin, systolic
blood pressure, diastolic blood pressure, BMI, pack-years smoking, and years of
education), a two-sample t test was used. When the baseline characteristics were clearly
non-Gaussian distributed, nonparametric analyses or parametric analyses on a suitably
2
transformed variable were performed. A analysis was used when the baseline
A general linear mixed model was used when evaluating the effects of blood pressure
control over time on kidney measures (creatinine clearance, serum creatinine, and log
UAE). Log UAE was used instead of UAE because of the non-Gaussian nature and large
variance of UAE values. The general linear mixed model is ideally suited for unbalanced
repeated-measures and longitudinal data. To further enhance understanding of the
longitudinal effects of blood pressure control on kidney function, t tests were carried out at
each time point. These tests are especially helpful in describing interactive effects between
blood pressure control and time. Progression of retinopathy and neuropathy were analyzed
2
using a test. Statistical significance was defined using = 0.05, and all values
RESULTS There were 470 hypertensive type 2 diabetic subjects included in the study.
Tables 1 and 2 show the baseline characteristics and prevalence of complications of the
study population according to those patients randomized to intensive versus moderate
antihypertensive therapy and those randomized to nisoldipine versus enalapril, respectively.
The baseline characteristics and interrelations of the ABCD population have been reported
in several publications (12,2834).
During the course of the study, a blood pressure separation was maintained between the
intensive and moderate therapy groups, which was achieved within the first 6 months and
then maintained for the remainder of the follow-up period (Fig. 2) (P < 0.001). The average
blood pressure for the last 4 years of follow-up was 132/78 mmHg for the intensive
antihypertensive therapy group and 138/86 mmHg for the moderate antihypertensive
therapy group. Figure 3 shows the mean systolic and diastolic blood pressure during the
follow-up period for patients randomized to nisoldipine versus enalapril in the intensive and
moderate arms of the study. There was no statistical difference in either group between the
enalapril and nisoldipine treatments. Over this time period, there was no difference between
glycosylated hemoglobin and total cholesterol when comparing the intensive
versusmoderate therapy group (Fig. 4A) and individuals randomized to nisoldipine versus
enalapril (Fig. 4B). HDL cholesterol, triglyceride, and LDL cholesterol levels between the
two groups were also not significantly different (data not shown).
Figure 2Systolic (A) and diastolic (B) blood pressures according to
intensive versus moderate therapy throughout 5 years. The t tests at each
time interval revealed that a significant blood pressure separation
occurred after 6 months between the two interventions (P < 0.001).
Figure 3Blood pressures throughout the 5 years according to enalapril versus nisolipine
therapy for those in the intensive (A) therapy group and the moderate (B) therapy group.
The t tests at each time interval revealed no significant difference between the therapies
The patients were on their initial randomized therapy an average of 70% of the study time.
There was no significant difference in the number of patients discontinuing study
medication between those randomized to nisoldipine and enalapril. The reasons for
discontinuing study medication include the following: adverse events (54 patients on
nisoldipine and 41 patients on enalapril); "voluntary" reasons (38 patients on nisoldipine
and 41 on enalapril, for reasons that include recommended to change to an ACE inhibitor
by their primary care physician, moved, or patient initiated); and death or cardiovascular
events (50 patients on nisoldipine and 41 on enalapril). Patients taken off enalapril (blinded)
and placed on open-label enalapril were still considered "off" study medication.
Figure 4Mean total cholesterol (normal range 130200 mg/dl) and glycohemoglobin
(normal range 4.27.0%) values over 5 years for intensive versus moderate therapy (A)
and nisoldipine versus enalapril therapy (B). The t tests at each time interval revealed no
significant difference between the therapies.
Nephropathy
Creatinine clearance. Repeated-measures analyses demonstrated that the change in
creatinine clearance and the log UAE throughout the 5-year follow-up period were not
significantly different between the intensive versus moderate therapy groups (Fig. 5). Using
a mixed model to perform a repeated-measures analysis also revealed that there is no
difference between intensive and moderate therapy as far as slope of creatinine clearance
over time. In the mixed model, the interaction between time and intervention (intensive vs.
moderate) was not significant. Subanalyses of creatinine clearance in patients starting with
normoalbuminuria and microalbuminuria revealed no differences between the intensive and
moderate antihypertensive therapy (Fig. 6). Virtually the entire decline in the mean
creatinine clearance occurred within the first year of the study for both the intensive and
moderate therapy groups with either normo- or microalbuminuria at baseline. Table 3
includes the percentage of patients that progressed from normoalbuminuria to
microalbuminuria or microalbuminuria to overt albuminuria. There was no significant
difference between the intensive and moderate therapy groups.
Compared with those patients with normo- or microalbuminuria at baseline, patients with
overt albuminuria (>300 mg/day) had a significant and continuous decline in creatinine
clearance throughout the 5-year period in both the intensive therapy (n = 46) and the
moderate therapy groups (n = 37). The t tests evaluating the change from baseline to 5 years
comparing intensive versus moderate therapy revealed no statistical difference (Table 4).
Figure 7 shows the mean creatinine clearance and log UAE for the patients randomized to
nisoldipine (n = 231) versus enalapril (n = 234) during the follow-up period. Neither the
mean nor the change in creatinine clearances was different between the two therapy groups.
Figure 7 presents lower mean log UAE values at 12, 18, 24, 36, and 42 months for patients
randomized to enalapril versus nisoldipine (P < 0.05). This difference in the mean of log
UAE was significant up to 3.5 years. In analyses stratified by level of intensity of blood
pressure reduction, there was no difference in the change in creatinine clearance and log
UAE between those randomized to nisoldipine versus enalapril (data not shown). Figure 8
shows the mean creatinine clearances for those patients starting with normo- and
microalbuminuria. There was no difference between those randomized to nisoldipine versus
enalapril. The mean creatinine clearances for patients with overt albuminuria are 74.9 4.9
at baseline to 53.3 ml min1 1.73 m2 at 5 years for the nisoldipine group and 77.2 4.9 at
baseline to 56.5 5.5 ml min1 1.73 m2 at 5 years for the enalapril group. These
decrements in creatinine clearance were not statistically different.
Figure 7Mean creatinine clearance and log UAE according to nisoldipine
versus enalapril therapy. The number of patients completing the creatinine
clearance measurements at each time period is listed on the bottom. *The t tests
demonstrate a difference in the mean of log UAE at 1, 1.5, 2, 3, and 3.5 years (P <
0.05).
Figure 8Mean creatinine clearance according to nisoldipine versus
enalapril therapy for patients with normoalbuminuria and
microalbuminuria at baseline. The number of patients completing the
creatinine clearance measurements at each time period is listed on the
bottom. The t tests evaluating change from baseline at each time interval
reveals no significant difference between the therapies.
Retinopathy
During the follow-up period, 30% of patients randomized to intensive therapy versus 34%
of patients randomized to moderate therapy progressed by three steps or more at 5 years (P
= 0.42). Using two-step progression, 39% of patients randomized to intensive therapy
versus 46% of patients randomized to moderate therapy progressed (P = 0.21).
During the follow-up period, 31% of patients randomized to nisoldipine versus 33% of
patients randomized to enalapril progressed by three steps or more at 5 years (P = 0.66).
Using two-step progression, 40% of patients randomized to enalapril versus 46% of patients
randomized to nisoldipine progressed (P = 0.30).
Neuropathy
During the follow-up period, 40% of patients randomized to intensive therapy versus 31%
of patients randomized to moderate therapy had progression of neuropathy at 5 years (P =
0.079). Subanalyses of autonomic neuropathy revealed that 18% of patients in the intensive
therapy group developed autonomic neuropathy versus 17% in the moderate therapy group
(NS).
During the follow-up period, 36% of patients randomized to nisoldipine versus 36% of
patients randomized to enalapril had progression of neuropathy at 5 years (P = 0.99).
Subanalyses of autonomic neuropathy revealed that 18% of patients in the nisoldipine
group developed autonomic neuropathy versus 17% in the enalapril group (NS).
With both intensive and moderate interventions, creatinine clearance remained relatively
stable over the 5-year follow-up period, with a small decline in creatinine clearance
occurring within the first year of treatment when compared with the last 4 years. In
subgroup analyses, creatinine clearance after 1 year stabilized in patients with normo- and
microalbuminuria at baseline. In contrast, patients with overt albuminuria at baseline
demonstrated a steady decline in creatinine clearance throughout the follow-up period of 5
6 ml min1 1.73 m2 per year, whether they were in the intensive or moderate treatment
group. This overall rate of decline for the ABCD Trial patients with overt albuminuria of 5
6 ml min1 1.73 m2 is similar to that reported by Flemming et al. (39) in a 42-month
follow-up period of hypertensive type 2 diabetic subjects with overt albuminuria and
considerably less than the 1012 ml min1 year1 observed without treatment of
hypertension (40).
More recently, the UKPDS demonstrated that tight blood pressure control (mean 144/82
mmHg) versus less tight control (mean 154/87 mmHg) resulted in less diabetes-related
deaths, cerebral vascular accidents, and combined microvascular complications (16). When
evaluating the effects on renal function in the UKPDS, tight blood pressure control resulted
in a lower urinary albumin concentration, but this difference was not apparent after year 6.
The blood pressure levels attained in the ABCD Trial for moderate therapy (138/86 mmHg)
were similar to the mean blood pressure in the tight blood pressure control group for the
UKPDS. On the other hand, the intensive treatment group in the ABCD Trial evaluated
blood pressures below those in the UKPDS. This intensive level of blood pressure control
(mean 132/78 mmHg) appeared to be quite safe in hypertensive type 2 diabetic patients
without any evidence of a "J curve." In the JNC-VI report, it was proposed that patients
with diabetes should have a blood pressure goal <130/85 mmHg (14). The results of the
intensive treatment group in the ABCD Trial are compatible with this recommendation and
appear to stabilize renal function if initiated before the presence of overt albuminuria (>300
mg/24 h).
Although the presence of microalbuminuria in type 1 diabetes has been a clear indicator of
inevitable renal failure if interventions are not performed, the role in type 2 diabetic
nephropathy is less clear. Mogensen (41) had originally demonstrated that only 22% of type
2 diabetic patients with microalbuminuria aged 5075 years developed proteinuria over a 9-
year follow-up period. Later studies in younger type 2 diabetic subjects suggest that the
development of overt nephropathy from microalbuminuria reaches 40% (42,43) but is still
much less than the 80% demonstrated in type 1 diabetic subjects. In the present study,
~20% of the patients advanced from normoalbuminuria to microalbuminuria and from
microalbuminuria to overt albuminuria over 5 years. There was however no difference
between intensive versus moderate blood pressure control. The absence of a difference
between the intensive versus moderate blood pressure control group suggests that a level of
blood pressure may have been reached in the moderate group, whereby a further reduction
exerts no additional benefit. Alternatively, it cannot be excluded that a larger group of
patients and/or a longer follow-up may demonstrate a more beneficial effect in the intensive
therapy group.
The present study demonstrated no statistical difference between the use of nisoldipine, a
long-acting CCB, versus enalapril, an ACE inhibitor, on diabetic nephropathy, as measured
by creatinine clearance and the log UAE over a 5-year follow-up period. However, an
initial advantage was observed with enalapril on the log UAE in the first 36 months. The
percentage of patients advancing from normo- to microalbuminuria and from
microalbuminuria to overt albuminuria was similar for both groups. Previous studies have
demonstrated the efficacy of ACE inhibition in diabetic nephropathy in both type 1 and type
2 diabetic subjects (39,4448). More recently, Ravid et al. (48) demonstrated that use of an
ACE inhibitor versus a placebo attenuated the decline in renal function and reduced the
extent of albuminuria in normotensive type 2 diabetic patients with normoalbuminuria over
a 6-year follow-up period.
As opposed to ACE inhibitors, the use of CCBs for diabetic nephropathy has been less
certain. Studies comparing the use of ACE inhibitors to CCBs have involved smaller study
populations with follow-up periods often <2 years (4547,4951). For the most part, the
results from these studies have suggested that use of an ACE inhibitor may be more
efficacious than a CCB based on UAE rates but without demonstrating an advantage on
glomerular filtration rates. The present study demonstrated a similar advantage of the ACE
inhibitor on UAE over the first 3.5 years of the study. There was no difference in creatinine
clearance between enalapril and nisoldipine in either the intensive or moderate treatment
group. The number of patients who eventually were off study medication at the end of the
present study is, however, a caveat.
Earlier studies have suggested that there is a positive relationship between hypertension and
the incidence or progression of diabetic retinopathy (8,5254). In the present study,
however, we did not demonstrate a significant difference on the progression of diabetic
retinopathy between intensive and moderate blood pressure control or between the use of a
CCB versus an ACE inhibitor over the 5-year follow-up. However, the larger UKPDS
demonstrated that over a 9-year follow-up, average blood pressure control of 144/82 mmHg
versus less control at 154/87 mmHg led to a decreased risk in the progression of
retinopathy. In the ABCD Trial, poor glycemic control may have contributed to the
progression of the retinopathy. It has been clearly demonstrated that tight glycemic control
slows the progression of diabetic retinopathy in both type 1 (55,56) and type 2 (57) diabetic
patients.
Of all the complications associated with diabetes, diabetic neuropathy is the most poorly
defined, but may be the most common. Cross-sectional studies suggest a relationship
between hypertension and the presence of neuropathy (58). Interventional studies with
regard to progression of neuropathy have involved glycemic control (55), aldose reductase
inhibitors (59), and -lipoic acid (60), but not antihypertensive therapy. In the present
In summary, the ABCD Trial suggests that creatinine clearance in hypertensive type 2
diabetic patients can be stabilized over 5 years with blood pressures maintained 132/78
138/86 mmHg if therapy is initiated before the onset of overt albuminuria. This supports the
JNC-VI recommendation of <130/85 mmHg for diabetic patients. These effects are
independent of the use of nisoldipine or enalapril as the initial antihypertensive medication.
Once diabetic nephropathy occurred (defined as >200 g/min [>300 mg/day] of
albuminuria), blood pressure control did not totally prevent loss of renal function, which
continued at a rate of 56 ml min1 1.73 m2 per year. In the current article, we also
observed no difference between intensive versus moderate blood pressure control and
enalapril versus nisoldipine with regard to the progression of diabetic retinopathy and
neuropathy over 5 years. Although the current article demonstrates no difference between
the use of a CCB versus an ACE inhibitor with regard to microvascular complications, the
use of an ACE inhibitor as the initial antihypertensive medication perhaps should be
preferred because of its possible advantage in macrovascular complications (20). Although
in need of further study, the intensive blood pressure control group demonstrated a decrease
in all-cause mortality.
References
1. Dupree EA, Meyer MB: Role of risk factors in complications of diabetes mellitus. Am J
Epidemiol 112:100112, 1980
2. Nelson RG, Newman JM, Knowler WC, Sievers ML, Kunzelman CL, Pettitt DJ, Moffett
CD, Teutsch SM, Bennett PH: Incidence of end-stage renal disease in NIDDM in Pima
Indians. Diabetologia 31:730746, 1988
3. Kannel WB, McGee DL: Diabetes and glucose tolerance as risk factors for
cardiovascular disease. Diabetes Care 2:120126, 1979
4. Walker WG, Hermann J, Murphy R, Patz A: Elevated blood pressure and angiotensin II
are associated with accelerated loss of renal function in diabetic nephropathy. Trans Am
Clin Climatol Assoc 97:94104, 1985
5. Christensen CK, Mogensen CE: The course of incipient diabetic nephropathy: studies of
albumin excretion and blood pressure. Diabet Med 2:97102, 1985
6. Parving HH, Andersen AR, Smidt UM, Oxenboll B, Edsberg B, Christiansen JS: Diabetic
nephropathy and arterial hypertension. Diabetologia 24:1012, 1983
7. Savage S, Schrier RW: Progressive renal insufficiency: the role of angiotensin converting
enzyme inhibitors. Adv Intern Med 37:85101, 1992
8. Knowler WC, Bennett PH, Ballantine EJ: Increased incidence of retinopathy in diabetes
with elevated blood pressure. N Engl J Med 301:645650, 1980
10. Klein R, Klein BE, Moss SE, Davis MD, DeMets DL: Is blood pressure a predictor of
the incidence or progression of diabetic retinopathy? Arch Intern Med 149:24272432,
1989
12. Mehler PS, Jeffers BW, Estacio R, Schrier RW: Associations of hypertension and
complications in non-insulin-dependent diabetes mellitus. Am J Hypertens 10:152161,
1997
14. Anonymous: The Sixth Report of the Joint National Committee on Prevention,
Detection, Evaluation, and Treatment of High Blood Pressure. Arch Intern Med 157:2413
2446, 1997
16. U.K. Prospective Diabetes Study Group: Tight blood pressure control and risk of
macrovascular and microvascular complications in type 2diabetes: UKPDS 38. BMJ
317:703713, 1998
17. Estacio RO, Savage S, Nagel NJ, Schrier RW: Baseline characteristics of participants in
the Appropriate Blood Pressure Control in Diabetes trial. Control Clin Trials 17:242257,
1996
18. Savage S, Johnson Nagel N, Estacio RO, Feig PU, MacCarthy EP, Lukken NJ, Ziegler
R, Schrier RW: The ABCD (Appropriate Blood Pressure Control in Diabetes) trial:
rationale and design of a trial of hypertension control (moderate or intensive) in type II
diabetes. Online J Curr Clin Trials 104:6250, 1993
19. Schrier RW, Savage S: Appropriate Blood Pressure Control in type 2 diabetes (ABCD
Trial): implications for complications. Am J Kidney Dis 20:653657, 1992
20. Estacio RO, Jeffers BW, Hiatt WR, Biggerstaff S, Gifford N, Schrier RW: The effect of
nisoldipine as compared with enalapril on cardiovascular outcomes in patients with non-
insulin-dependent diabetes and hypertension. N Engl J Med 338:645652, 1998
21. World Health Organization: Diabetes Mellitus: Report of a WHO Study. Geneva, World
Health Org., 1985 (Tech. Rep. Ser., no. 727)
22. Early Treatment Diabetic Retinopathy Study Research Group: Grading diabetic
retinopathy from stereoscopic color fundus photographs: an extension of the Modified
Airlie House Classification: ETDRS report number 10. Ophthalmology 98:786806, 1991
23. Consensus Panel: Report and recommendations of the San Antonio Conference on
Diabetic Neuropathy. Ann Neurol 24:99106, 1988
24. Mogensen CE: Microalbuminuria in diabetic renal disease. In Prevention and Treatment
of Diabetic Late Complications. Mogensen CE, Standl E, Eds. New York, Walter de
Gruyter, 1989, p. 4173
25. Savage S, Snyderm R, Feig PU, Lukken N, Schrier RW: ABCD Trial: simultaneous
iothalamate and creatinine clearance compared to Cockcroft Gault formula for estimating
glomerular filtration rate (GFR) in type II diabetes mellitus (Abstract). Am Soc Nephrol
1993
26. Early Treatment Diabetic Retinopathy Study Research Group: Fundus photographic risk
factors for progression of diabetic retinopathy: ETDRS report no. 12. Ophthalmology
98:823833, 1991
28. Cohen JA, Jeffers BW, Faldut D, Marcoux M, Schrier RW: Risks for sensorimotor
peripheral neuropathy and autonomic neuropathy in non-insulin-dependent diabetes
mellitus (NIDDM). Muscle Nerve 21:7280, 1998
29. Estacio RO, Wolfel EE, Regensteiner JG, Jeffers B, Havranek EP, Savage S, Schrier
RW: Effect of risk factors on exercise capacity in NIDDM. Diabetes 45:7985, 1996
30. Estacio RO, McFarling E, Biggerstaff S, Jeffers BW, Johnson D, Schrier RW: Overt
albuminuria predicts diabetic retinopathy in Hispanics with NIDDM. Am J Kidney Dis
31:947953, 1998
31. Jeffers BW, Estacio RO, Raynolds MV, Schrier RW: Angiotensin-converting enzyme
gene polymorphism in non-insulin dependent diabetes mellitus and its relationship with
diabetic nephropathy. Kidney Int 52:473477, 1997
32. Savage S, Nagel NJ, Estacio RO, Lukken N, Schrier RW: Clinical factors associated
with urinary albumin excretion in type 2 diabetes. Am J Kidney Dis 25:836844, 1995
33. Savage S, Estacio RO, Jeffers B, Schrier RW: Urinary albumin excretion as a predictor
of diabetic retinopathy, neuropathy, and cardiovascular disease in NIDDM. Diabetes Care
19:12431248, 1996
34. Savage S, Estacio RO, Jeffers B, Schrier RW: Increased complications in noninsulin-
dependent diabetic patients treated with insulin versus oral hypoglycemic agents: a
population study. Proc Assoc Am Physicians 109:181189, 1997
35. Pell S, D'Alonzo CA: Some aspects of hypertension in diabetes mellitus. JAMA
202:104110, 1967
38. National Institute of Diabetes and Digestive and Kidney Diseases: Incidence and
prevalence of ESRD. In United States Renal Data System 1998 Annual Data Report.
Chapter 2. Bethesda, MD, National Institutes of Health, p. 2335, 1998
39. Flemming SN, Rossing P, Gall MA, Skott P, Smidt UM, Parving HH: Long-term effect
of lisinopril and atenolol on kidney function in hypertensive NIDDM subjects with diabetic
nephropathy. Diabetes 46:11821188, 1997
40. Parving HH: The impact of hypertension and antihypertensive treatment on the course
and prognosis of diabetic nephropathy. J Hypertens 8:S187S191, 1990
41. Mogensen CE: Microalbuminuria predicts clinical proteinuria and early mortality in
maturity-onset diabetes. N Engl J Med 310:356360, 1984
42. Nelson RG, Bennett PH, Beck GJ, Tan M, Knowler WC, Mitch WE, Hirschman GH,
Myers BD: Development and progression of renal disease in Pima Indians with non-
insulin-dependent diabetes mellitus: Diabetic Renal Disease Study Group. N Engl J Med
335:16361642, 1996
43. Ravid M, Savin H, Jutrin I, Bental T, Katz B, Lishner M: Long-term stabilizing effect of
angiotensin-converting enzyme inhibition on plasma creatinine and on proteinuria in
normotensive type II diabetic patients. Ann Int Med 118:577581, 1993
44. Lewis EJ, Hunsicker LG, Bain RP, Rohde RD: The effect of angiotensin-converting
enzyme inhibition on diabetic nephropathy. N Engl J Med 118:577583, 1993
46. Chan JCN, Cockram CS, Nicholls MD, Cheung CK, Swaminathan R: Comparison of
enalapril and nifedipine in treating non-insulin-dependent diabetes associated with
hypertension: one-year analysis. BMJ 305:981985, 1992
49. Rossing P, Tarnow L, Boelskifte S, Jensen BR, Nielsen FS, Parving HH: Differences
between nisoldipine and lisinopril on glomerular filtration rate and albuminuria in
hypertensive IDDM patients with diabetic nephropathy during the first year of treatment.
Diabetes 46:481487, 1997
50. Bretzel RG, Bollen CC, Maser E, Federlin KF: Nephroprotective effects of nitrendipine
in hypertensive type I and type II diabetic patients. Am J Kidney Dis 21:5364, 1993
51. Parving HH, Rossing P: The use of antihypertensive agents in prevention and treatment
of diabetic nephropathy. Curr Opin Nephrol Hypertens 3:292300, 1994
52. Chahal P, Inglesby DV, Sleightholm M, Kohner EM: Blood pressure and the
progression of mild background diabetic retinopathy. Hypertension 7 (Suppl. 2):7983,
1985
53. Moss SE, Klein R, Klein BEK: Ocular factors in the incidence and progression of
diabetic retinopathy. Ophthalmology 101:7783, 1994
54. Klein BEK, Klein R, Moss SE, Palta M: A cohort study of the relationship of diabetic
retinopathy to blood pressure. Arch Ophthalmol 113:601606, 1995
55. DCCT Research Group: The effect of intensive treatment of diabetes on the
development and progression of long-term complications in insulin-dependent diabetes
mellitus. N Engl J Med 329:977986, 1993
58. Knuiman MW, Welborn TA, McCann VJ, Stanton KG, Constable IJ: Prevalence of
diabetic complications in relation to risk factors. Diabetes 35:13321339, 1986
60. Ziegler D, Hanefeld M, Ruthnau KJ, Meissner HP, Lobisch M, Schutte K, Gries FA:
Treatment of symptomatic diabetic peripheral neuropathy with the anti-oxidant alpha-lipoic
acid. Diabetologia 38:14251433, 1995
Address correspondence and reprint requests to Robert W. Schrier, MD, Division of Renal
Diseases and Hypertension, Department of Medicine, 4200 E. Ninth Ave., #B178, Denver,
CO 80262. E-mail: robert.schrier@uchsc.edu.
Received for publication 9 July 1999 and accepted in revised form 7 December 1999.
A table elsewhere in this issue shows conventional and Systme International (SI) units and
conversion factors for many substances.
This article is based on a presentation at a symposium. The symposium and the publication
of this article were made possible by an unrestricted educational grant from Aventis
Pharma.