Diabetic Nephropathy Clinical Trial
Thiamine is a key component in the creation of physiologic anti-inflammatory mediators. Serum thiamine stores have been found to be deficient in diabetic patients. Thiamine deficiency may be a key pathological mechanism of inflammation that results in diabetic kidney and retinal injury. The investigators hypothesize that the repletion of a patient's thiamine by oral supplementation may result in reduced inflammation, and therefore reduced kidney injury.
Thiamine (vitamin B1) is a water-soluble vitamin. It is absorbed from the gastrointestinal
tract and taken up into tissues by transport proteins and converted to thiamine
pyrophosphate (TPP) by thiamine pyrophosphokinase (TPPK). TPP is a co-factor of pyruvate
dehydrogenase (PDH), α-ketoglutarate dehydrogenase and transketolase (TKT)—enzymes involved
in the metabolism of glucose.
Various transport proteins are involved in the transport of thiamine monophosphate (TMP) and
TPP across membranes. These include thiamine transported isoform-1 (THTR1) and thiamine
transporter isoform-2 (THTR2), reduced folate carrier-1 (RFC-1), which transports TMP and
TPP across cell plasma membranes and the mitochondrial TPP transporter (mTHTR). Thiamine and
TMP/TPP transporters may have abnormal expression in diabetes. Increased THTR1 levels are
found in red blood cells (RBCs) and mononuclear leucocytes of patients with diabetes
compared to those of healthy subjects. RBC precursors and leucocytes appeared to up-regulate
THTR1 expression in response to decreased thiamine availability. In the presence of
hyperglycemia, renal tubular epithelial cells, by contrast, have decreased expression. In
both experimental models of diabetes and in human diabetics increased clearance of thiamine
has been demonstrated. This precedes the development of microalbuminuria. Patients with
microalbuminuria and early decline in glomerular filtration rate had higher fractional
excretion of thiamine compared to patients with stable renal function.
Thiamine supplementation in STZ- diabetic mice prevented the development of
microalbuminuria, decreasing urinary albumin excretion (UAE) by approximately 80%. In
addition thiamine supplementation prevented diuresis and glycosuria. Human studies are
limited but in one placebo controlled study the thiamine group showed a significant decrease
in microalbuminuria in diabetic patients on thiamine.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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