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Current Diabetes Reviews
ISSN: 1573-3998
Current Diabetes Reviews
Volume 3, Number 2, May 2007
Contents
Progression of Retinopathy in Type 1 Diabetic Women
During Pregnancy Pp. 85-93
Risto Kaaja and Sirpa Loukovaara
[Abstract]
Management of Obesity in Patients with Type 2
Diabetes Mellitus Pp. 95-101
Lucia Gagliardi and Gary Wittert
[Abstract]
Diabetic Vasculopathy and the Lectin-Like Oxidized
Low-Density Lipoprotein Receptor-1 (LOX-1) Pp. 103-110
Geneviève Renier, Fritz Maingrette and Ling Li
[Abstract]
“Actin” g on GLUT4: Membrane & Cytoskeletal
Components of Insulin Action Pp. 111-122
Joseph T. Brozinick, Jr., Bradley A. Berkemeier and Jeffrey
S. Elmendorf
[Abstract]
Highest Mortality During the Last Year Before and
the First Year After Start of Dialysis Treatment in Type 2
Diabetic Patients with Nephropathy Pp. 123-126
Georg Biesenbach
[Abstract]
Comparative Effectiveness of Pioglitazone and Rosiglitazone
in Type 2 Diabetes, Prediabetes, and the Metabolic Syndrome:
A Meta-Analysis Pp. 127-140
Susan L. Norris, Susan Carson and Carol Roberts
[Abstract]
Reducing the Risk of Type 2 Diabetes – Early
Identification of High-Risk Individuals and Treatment with
Acarbose Pp. 141-148
Chang-Yu Pan
[Abstract]
Abstracts
[Back to top]
Progression of Retinopathy in Type 1 Diabetic Women
During Pregnancy
Risto Kaaja and Sirpa Loukovaara
Progression of diabetic retinopathy (DR) occurs at least
temporarily during pregnancy and postpartum. The pathogenetic
mechanisms of DR progression during pregnancy are not fully
understood. Several factors related to metabolic changes (hyperglycaemia),
diabetes itself (duration of diabetes before conception, baseline
status of DR), pregnancy physiology (hypervolaemia and hypercoagulation,
impaired retinal autoregulation) and pregnancy complications
(pre-eclampsia) seem to play important roles in the progression
of DR during pregnancy. On the other hand, systemic angiopoietic
and vasoactive factors seem to have minor role in the deterioration
of DR during that time period. Good glycaemic control, normotension,
lack of nephropathy as well as lack of pre-proliferative/proliferative
changes of DR are good prognostic factors as regards the progression
of DR during pregnancy. However, pregnancy seems to have no
long-term detrimental effects as regards the progression of
DR unless it has proceeded to pre-proliferative and proliferative
phases.
[Back to top]
Management of Obesity in Patients with Type 2
Diabetes Mellitus
Lucia Gagliardi and Gary Wittert
Type 2 Diabetes Mellitus (T2DM) is a disease of over nutrition;
the onset and progression of which, is associated with excess
fat accumulation in the abdomen, muscles and liver. In this
review, we focus on management of obesity as the primary strategy
for management of disorders of glucose metabolism. Modest
weight loss (~7%) achieved by diet and exercise can prevent,
or delay, the onset of T2DM. In those with established T2DM,
weight loss reduces fasting and post-prandial plasma glucose
levels, HbA1c, and the need for pharmacotherapy. The beneficial
effects on glucose metabolism of caloric restriction, and
aerobic and resistance exercise, may occur independently of
weight loss. When substantial weight loss is required, meal
replacements allow a large reduction in energy consumption
whilst maintaining micronutrient intake. Pharmacotherapy for
obesity, as part of an integrated management plan, is useful
for maintaining weight loss and optimising glycaemic control.
The most effective long-term therapy for obesity remains bariatric
surgery, which is associated with resolution of T2DM in over
80% of patients.
The currently available pharmacotherapies for T2DM mostly
result in weight gain. Pramlintide and exenatide are new therapies
which hold promise, because in addition to improved glycaemic
control, they also result in weight loss.
[Back to top]
Diabetic Vasculopathy and the Lectin-Like Oxidized
Low-Density Lipoprotein Receptor-1 (LOX-1)
Geneviève Renier, Fritz Maingrette and Ling Li
Type 2 diabetes is associated with an increased incidence
of coronary heart disease and cardiovascular complications.
One crucial step in the initiation and progression of atherosclerosis
is the unregulated uptake of oxidized low-density lipoprotein
(oxLDL) by vascular wall components through scavenger receptors.
Identification of lectin-like oxidized low-density lipoprotein
receptor-1 (LOX-1) as the major receptor for oxLDL in endothelial
cells has provided a new clue to the mechanisms involved in
oxLDL accumulation in the vessel wall. This receptor, by facilitating
the uptake of oxLDL, induces endothelial dysfunction and mediates
numerous oxLDL-induced proatherogenic effects. Besides endothelial
cells, LOX-1 is also expressed by smooth muscle cells and
macrophages. In these cells, LOX-1 may function as a scavenger
receptor and promote foam cell formation. Notably, LOX-1 is
induced by multiple stimuli relevant to atherogenesis and
inflammation and is up-regulated in various proatherogenic
conditions, including diabetes. As such, activation of vascular
cells by oxLDL through LOX-1 may be relevant to the development
and progression of human diabetic vasculopathy. This review
summarizes recent advances related to the role of LOX-1 in
atherosclerosis, its regulation by metabolic and inflammatory
factors relevant to diabetes and the impact of these factors
on LOX-1-mediated proatherogenic events linked to diabetic
vasculopathy.
[Back to top]
“Actin” g on GLUT4: Membrane & Cytoskeletal
Components of Insulin Action
Joseph T. Brozinick, Jr., Bradley A. Berkemeier and Jeffrey
S. Elmendorf
The dissection of mechanisms that regulate glucose transport
by insulin has revealed an intricate network of signaling
molecules scattered from the insulin receptor to the intracellular
glucose transporter GLUT4. It is also appreciated that some
insulin receptor signals jaunt in different directions to
regulate events essential for the efficient redistribution
of GLUT4 to the plasma membrane. Moreover key assists in the
process appear to be arranged by membrane lipids and cytoskeletal
proteins. Following current considerations of insulin signals
regulating GLUT4, this review will focus on in vitro
and in vivo evidence that supports an essential role
for phosphoinositides and actin filaments in the control of
glucose transport. The discussion will visit recent cell culture,
whole animal, and human data highlighting membrane and cytoskeletal
aspects of insulin resistance.
[Back to top]
Highest Mortality During the Last Year Before and
the First Year After Start of Dialysis Treatment in Type 2
Diabetic Patients with Nephropathy
Georg Biesenbach
Purpose of review: The mortality of type 2 diabetic
patients with renal disease is high during both the pre-dialysis
period as well as the period under dialysis therapy. With
respect to rare data in the literature it may be assumed that
the mortality rate is especially high during the last year
before and the first year after start of dialysis therapy.
Recent findings: After reviewing the reports in the
literature dealing with survival of diabetic patients with
nephropathy it may be concluded that mortality is especially
high during the year before and after initiating dialysis.
There are exact survival data of type 2 diabetic patients
under dialysis therapy but only few data concerning the survival
during the last year prior to dialysis treatment. The possible
reasons for this higher mortality shortly before and after
start of dialysis are discussed in this article. Summary:
The mortality in type 2 diabetic patients is especially high
during the last year before and the first year after the start
of dialysis therapy. However, only the higher mortality during
the first year after initiating dialysis is well documented
in the literature. Those patients who die early within 90
days of dialysis are not registered in the registries, therefore,
the overall mortality during the first dialysis year is at
least 5% higher than the registered. uring both periods several
factors may play a causal role in the high mortality, a higher
prevalence of heart failure, and a progression of macroangiopathy
with higher incidence of cardiovascular events due to traditional
and non-traditional risk factors, especially inflammation
and oxidative stress.
[Back to top]
Comparative Effectiveness of Pioglitazone and Rosiglitazone
in Type 2 Diabetes, Prediabetes, and the Metabolic Syndrome:
A Meta-Analysis
Susan L. Norris, Susan Carson and Carol Roberts
Objective - To assess the comparative efficacy and
safety of pioglitazone and rosiglitazone.
Research design and methods – Multiple electronic
databases were searched for randomized, controlled trials
(RCTs) of efficacy or effectiveness and for studies of any
design which reported adverse events. Pooled estimates were
calculated using a random effects model.
Results - Eighty-seven RCTs fulfilled our inclusion
criteria for efficacy or effectiveness and 42 studies examined
safety or tolerability. Two head-to-head RCTs of type 2 diabetes
demonstrated significant improvements in A1c in both groups
at follow-up with no significant difference between groups;
a third study found no significant change in A1c in either
group. The pooled estimate of effect on A1c for pioglitazone
compared to placebo was -0.99% (95% confidence interval [CI],
-1.18, -0.81) and for rosiglitazone was -0.92% (95% CI, -1.2,
-0.64). Indirect comparison revealed no significant difference
in A1c (between-drug difference -0.07% [95% CI, -0.41, 0.27]).
Rosiglitazone increased total cholesterol compared to pioglitazone
(net between-drug effect 13.91 mg/dl [95% CI, 1.20 to 26.62]).
Both drugs increased weight by 2 to 3 kg and rates of adverse
events were similar for the two drugs. Data were insufficient
to assess comparative effects on health outcomes such as cardiovascular
events.
Conclusions - Based largely on indirect evidence,
the two thiazolidinediones appear to have similar effects
on glycemic control and similar side-effect profiles. Rosiglitazone
may increase total cholesterol compared to pioglitazone. Studies
are needed which provide direct comparisons between the two
drugs, particularly for long-term health outcomes.
[Back to top]
Reducing the Risk of Type 2 Diabetes – Early
Identification of High-Risk Individuals and Treatment with
Acarbose
Chang-Yu Pan
The severity of the type 2 diabetes epidemic is widely acknowledged.
Demographic, social, and cultural changes around the world
are driving a dramatic increase in the prevalence of type
2 diabetes. Consequently, there is increasing interest in
defining the target population and developing strategies for
preventing or delaying the disease. Impaired glucose tolerance
(IGT), an asymptomatic condition early in the disease continuum
of dysglycemia, is the best target for intervention, as it
is a strong predictor for the development of both type 2 diabetes
and cardiovascular disease (CVD). Identifying individuals
likely to have IGT using risk-prediction tools is simple and
cost-effective; diagnosis can be confirmed with an oral glucose
tolerance test. Numerous trials have examined the benefits
of intervention in IGT populations. Lifestyle modification
and some pharmacologic therapies, such as acarbose, have been
shown to significantly reduce disease progression. Acarbose
therapy has also been associated with significant reductions
in cardiovascular events and new cases of hypertension. Trials
assessing the potential preventive effects of various therapies
are ongoing, but current evidence confirms that early intervention
in individuals with IGT can reduce the risks of type 2 diabetes
and CVD. Identification of high-risk individuals should therefore
be standard in general practice and, if IGT is diagnosed,
therapeutic intervention should be initiated promptly.
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