Cystatin C and Fibrinogen Plasma Levels as early Predictors of Diabetic Nephropathy in Type II Diabetes Mellitus; a Review Article
Wedad Alruwaytie, Amal Mackawy, Ali Abu-Dahash
716
ABSTRACT
Background: Diabetic
nephropathy (DN) is a dangerous illness associated with a significant risk for
cardiovascular and kidney problems in diabetic patients. Serum cystatin C
levels may rise in diabetic individuals with microalbuminuria, and it has been
recommended as an endogenous glomerular filtration rate (GFR) marker because of
its link to the albumin to creatinine ratio (ACR) in diabetic nephropathy.
Uncontrolled diabetes was found to have a greater level of fibrinogen; in
diabetic nephropathy, fibrinogen levels are important. In addition, fibrinogen
has been associated to inflammation and has been demonstrated to play a crucial
pathophysiologic role in the advancement of renal impairment in individuals.
Methods: The author has no
intention of commenting on the molecular role of cystatin C, a cysteine
protease inhibitor, or the disrupted haemostatics mechanism in
fibrinogen-induced diabetes. in this
study, which is expected to investigate views on using the cystatin C as
well as plasma fibrinogen plasma levels like an early markers of nephrotic
syndrome. Therefore, 4 important clinical datasets were reviewed,
including the EMBASE, PubMed and The Cochrane Library, Medline, Google Scholar
and a few additional related journals datasets, as well as relevant records
were collected with high precision.
Conclusion: When
compared to the frequently used creatinine-based predictions, cystatin C is a
good marker for diagnosing nephropathy in patients with normal albuminuria, and
it may enhance the risk prediction in diabetics. Even before the complication of
chronic kidney disease symptoms, Cystatin C levels in urine might be raised in
diabetic individuals. Additional investigation into cystatin C and fibrinogen
functions as early biomarkers, clinical value in screening, involvement in
prognosis, decrease of inflammation and prediction of medication clearance, and
drug monitoring in type II diabetic, nephropathy is needed.
Keywords: cystatin
C, fibrinogen, nephropathy, diabetes mellitus, biomarkers
ABSTRACT
Background: Diabetic
nephropathy (DN) is a dangerous illness associated with a significant risk for
cardiovascular and kidney problems in diabetic patients. Serum cystatin C
levels may rise in diabetic individuals with microalbuminuria, and it has been
recommended as an endogenous glomerular filtration rate (GFR) marker because of
its link to the albumin to creatinine ratio (ACR) in diabetic nephropathy.
Uncontrolled diabetes was found to have a greater level of fibrinogen; in
diabetic nephropathy, fibrinogen levels are important. In addition, fibrinogen
has been associated to inflammation and has been demonstrated to play a crucial
pathophysiologic role in the advancement of renal impairment in individuals.
Methods: The author has no
intention of commenting on the molecular role of cystatin C, a cysteine
protease inhibitor, or the disrupted haemostatics mechanism in
fibrinogen-induced diabetes. in this
study, which is expected to investigate views on using the cystatin C as
well as plasma fibrinogen plasma levels like an early markers of nephrotic
syndrome. Therefore, 4 important clinical datasets were reviewed,
including the EMBASE, PubMed and The Cochrane Library, Medline, Google Scholar
and a few additional related journals datasets, as well as relevant records
were collected with high precision.
Conclusion: When
compared to the frequently used creatinine-based predictions, cystatin C is a
good marker for diagnosing nephropathy in patients with normal albuminuria, and
it may enhance the risk prediction in diabetics. Even before the complication of
chronic kidney disease symptoms, Cystatin C levels in urine might be raised in
diabetic individuals. Additional investigation into cystatin C and fibrinogen
functions as early biomarkers, clinical value in screening, involvement in
prognosis, decrease of inflammation and prediction of medication clearance, and
drug monitoring in type II diabetic, nephropathy is needed.
Keywords: cystatin
C, fibrinogen, nephropathy, diabetes mellitus, biomarkers