关于糖尿病肾病治疗新方法的项目工作

Purushottam Ravindra Patil, Nikhil Kailas Patil, V. Khairnar
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摘要

肾功能衰竭是糖尿病常见的长期并发症。糖尿病肾病的阶段已经被描述为其临床病程的特征。糖尿病肾病继发于损害肾小球的长期改变。以控制肾小球压力和全身性高血压为重点的治疗可以减缓蛋白尿的进展和肾功能的恶化。血管紧张素转换酶(ACE)抑制剂和钙通道阻滞剂已被证明是有效的管理糖尿病肾病。对糖尿病患者采取系统的方法,有助于在病程早期识别那些个体,此时适当的治疗可能最有帮助。糖尿病肾病是慢性肾脏疾病的主要原因,也是心血管疾病死亡的主要原因。糖尿病肾病可分为微量蛋白尿和大量蛋白尿。微观和宏观蛋白尿的临界值是任意的,它们的值一直受到质疑。蛋白尿在高正常范围内的受试者似乎有高风险进展为微量或巨量蛋白尿,并且他们的血压也高于正常蛋白尿在低正常范围内的受试者。糖尿病肾病的筛查是通过测定尿白蛋白来进行的。如果不正常,应在三至六个月的时间间隔内采集三份样本中的两份进行确认。此外,建议常规估计肾小球滤过率,以适当筛查肾病,因为有些患者在尿白蛋白值处于正常范围时肾小球滤过率下降。糖尿病肾病的两个主要危险因素是高血糖和动脉高血压,但1型和2型糖尿病的遗传易感性非常重要。其他危险因素包括吸烟、血脂异常、蛋白尿、肾小球高滤过和饮食因素。1型糖尿病患者肾病的病理特征是肾小球和肾小管基底膜增厚,伴有进行性脑膜扩张(弥漫性或结节性),导致肾小球滤过表面进行性减少。传入和传出肾小球小动脉同时发生间质形态改变和透明化。足细胞异常似乎也与肾小球硬化过程有关。2型糖尿病患者的肾脏病变是异质性的,比1型糖尿病患者更复杂。糖尿病肾病的治疗是基于多种危险因素的方法,其目标是延缓疾病的发展或进展,并降低受试者增加的心血管疾病风险。实现最佳代谢控制,治疗高血压(<130/80 mmHg)和血脂异常(LDL胆固醇<100 mg/dl),使用阻断肾素-血管紧张素-醛固酮系统的药物,是预防微量蛋白尿发展,延缓肾病进展到更晚期,降低糖尿病患者心血管死亡率的有效策略。
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A Project work on Recent approches in the Treatment of Diabetic Nepheropathy
Renal failure is a common long-torm complication of diabetes mellitus. Stages of diabetic nephropathy have been described that characterize its clinical course. Diabetic nephropathy develops secondary to long- changes that damage the glomeruli’s. Therapy that focuses on the control of glomerular pressures and systemic hypertension can slow the progression of proteinuria and deterioration of renal function. Angiotensin converting enzyme (ACE) inhibitors and calcium channel blockers have been demonstrated to be effective in the management of diabetic nephropathy. A systematic approach to the patient with diabetes with help identify those individuals early in the course of disease when proper therapy may be most helpful. Diabetic nephropathy is the leading cause of chronic renal disease and a major cause of cardiovascular mortality. Diabetic nephropathy has been categorized into stages: micro albuminuria and macro albuminuria. The cut-off values of micro- and macro albuminuria are arbitrary and their values have been questioned. Subjects in the upper-normal range of albuminuria seem to be at high risk of progression to micro- or macro albuminuria and they also had a higher blood pressure than normoalbuminuric subjects in the lower norm albuminuria range. Diabetic nephropathy screening is made by measuring albumin in spot urine. If abnormal, it should be confirmed in two out three samples collected in a three to six-months interval. Additionally, it is recommended that glomerular filtration rate be routinely estimated for appropriate screening of nephropathy, because some patients present a decreased glomerular filtration rate when urine albumin values are in the normal range. The two main risk factors for diabetic nephropathy are hyperglycemia and arterial hypertension, but the genetic susceptibility in both type 1 and type 2 diabetes is of great importance. Other risk factors are smoking, dyslipidemia, proteinuria, glomerular hyper filtration and dietary factors. Nephropathy is pathologically characterized in individuals with type 1 diabetes by thickening of glomerular and tubular basal membranes, with progressive meningeal expansion (diffuse or nodular) leading to progressive reduction of glomerular filtration surface. Concurrent interstitial morphological alterations and hyalinization of afferent and efferent glomerular arterioles also occur. Podocytes abnormalities also appear to be involved in the glomerulosclerosis process. In patients with type 2 diabetes, renal lesions are heterogeneous and more complex than in individuals with type 1 diabetes. Treatment of diabetic nephropathy is based on a multiple risk factor approach, and the goal is retarding the development or progression of the disease and to decrease the subject's increased risk of cardiovascular disease. Achieving the best metabolic control, treating hypertension (<130/80 mmHg) and dyslipidemia (LDL cholesterol <100 mg/dl), using drugs that block the renin-angiotensin-aldosterone system, are effective strategies for preventing the development of micro albuminuria, delaying the progression to more advanced stages of nephropathy and reducing cardiovascular mortality in patients with diabetes.
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