Diabetic nephropathy:
Diabetes mellitus is a chronic
hyperglycemia sufficient to cause multisystem dysfunction but mostly retina,
kidney, nerves and arteries. Type 1 DM is due to autoimmune destruction of
pancreatic islet beta cells causing loss of insulin. Type 2 diabetes is due to
combination of cellular resistance to insulin and beta cell failure.
Diabetic nephropathy (DN) there is
finding of proteinuria in patient with diabetes with no evidence of UTI. Overt
nephropathy occurs when albumin excretion of around 300 mg/day. Albumin
measurement in urine is the recommended for detecting and monitoring kidney damage
in adults. Patients with albuminuria 30-300 mg/day are said to be having
microabluminuria.
In DN, there is kidney necrosis,
contraction, thickened basement membrane and other abnormalities. Clinical
progression is defined in terms of change in urinary albumin excretion rate and
decline in GFR and blood pressure. In type 1 DM, microabluminuria develops
later after 5 years of diagnosis or at any time after 40 years of age. So
annual monitoring or urine albumin is recommended after 5 years disease duration.
Type 2 DM are usually older at presentation and defining the date of onset is
difficult and annual monitoring of urine albumin is recommended from the time
of diagnosis.
Hyperinfiltration with progressive
increase in UAE with decrease in GFR can lead to hypertension and finally cause
ESRD with uraemic syndrome.
To this date the best available
predictor for development of nephropathy in kidney disease and in diabetics, is
microabluminuria as UAE represents generalized vascular damage than renal
microvascular injury alone.
The exact mechanism for
hyperglycemic tissue damage probably includes
a. Formation
of Advanced glycation end products (AGE)
b. Overactivity
of polyol pathway. Polyols are sugar alcohols formed from their respective
sugars under the action of aldose reductase.
c. Generation
of ROS
Glucose is preferentially shunted
through the polyol pathway under hyperglycemic conditions generating sorbitol
that accumulates within cells. Abundance of glucose and its product in ECM of
glomerulus and interstitium is a key step in pathogenesis. There is excess of
ECM within glomeruli and interstitium. E.g. TGF-β is stimulated by
hyperglycemia, AGE, angiotensin II and ROS this TGF-β cause the upregulation of
insulin independent GLUT-1 transporter in mesangial cells. Glucose is
transported to cells through GLUT-1 and metabolized mainly be glycolytic
pathway. Activation of other signaling pathways like PKC, DAG, MAPK, etc.
induces expression of ECM proteins. Hypersclerotic and hypertrophic effect of
glucose are largely mediated by TGFβ which is seen to be overproduced in DN
patients.
The receptors for AGE has been
identified (RAGE) which is selectively expressed in glomerular epithelial cells
(podocytes). Increased accumulation of AGE in diabetes engages podocyte RAGE
and may lead to increased glomerular permeability. Vascular permeability a
hallmark of diabetes can be suppressed by inhibiting RAGE in animal model.
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