Ranjan Mala, Nayak Sujatha, Rao Beedu Sashidhar
Department of Biochemistry, University College of Science, Osmania University, Hyderabad, India.
Mol Vis. 2006 Sep 13;12:1077-85.
This study used an immunochemical approach aimed to detect the glycated crystallins (beta- and gamma-crystallin) in rat lens and their circulating specific autoantibodies in serum during the course of cataractogenesis.
Streptozocin (STZ; 55 mg/kg body mass) induced diabetic male Wistar/NIN rats (2-3 months old) and control nondiabetic rats were used for this study. Plasma glucose, glycated hemoglobin and body weight were evaluated on day zero, and at the interval of every two weeks up to the eighth week of post-injection in both the groups. Other biochemical parameters, such as the levels of nonprotein sulfhydryl (-SH) groups and the activity of gamma-glutamyl transpeptidase (gamma-GT) in lens proteins were also estimated. Cataract progress was monitored by measuring the advanced glycation end product (AGE)-like fluorophores in both intact lens as well as in lens homogenate employing digital based image analysis and spectrofluorimetric methods. Similarly, the polyclonal antibodies specific to beta-glycated-, gamma-glycated-, beta-, and gamma-crystallins were used to determine the concentration of respective immunogens in lens by noncompetitive ELISA and their respective circulating antibodies by antibody capture assay. The profile of glycated lens protein (soluble and insoluble fractions) during the course of cataractogenesis was assessed by the western blot technique.
STZ induced diabetic rats showed typical signs of diabetes (hyperglycemia, increased water and food intake with no increase in body weight). Biochemical analysis of total lens protein showed a significant (p = <0.001) decrease in the levels of nonprotein -SH groups. The activity of lenticular gamma-GT in diabetic rats was found to be unaltered as compared to the control group. Digital analysis of intact lens illustrated a positive correlation (r(2)=0.888) with the formation of AGE-like fluorophores during the course of cataractogenesis. A similar trend was also observed in the levels of AGE-like fluorophores in the total lens homogenate of diabetic animals during the course of cataractogenesis. The concentration of beta- and gamma-glycated-crystallins in the rat lens (soluble and insoluble fractions) was analyzed by non-competitive ELISA. The concentration of beta- and gamma-glycated-crystallins were found to be enhanced by the end of week eight, as compared to the control group. Concomitantly, crystallin-specific (beta- and gamma-glycated-crystallin) autoantibodies were also detected in the serum of the diabetic rats from week two onwards. Western blot analysis indicated the formation of enhanced glycated lens crystallins (beta- and gamma-crystallin) in the insoluble fraction.
The following was observed during the course of cataractogenesis: (1) there was an enhanced formation of AGEs-like fluorophores in intact lens; (2) beta- and gamma-glycated-crystallin levels increased in the rat lens (insoluble fraction) by the end of week eight; and (3) release of these glycated lens proteins into peripheral circulation resulted in the production of autoantibodies to beta- and gamma-glycated-crystallins that could be detected as early as week two, after induction of diabetic status in experimental rats.
本研究采用免疫化学方法,旨在检测大鼠晶状体中的糖化晶状体蛋白(β-和γ-晶状体蛋白)及其在白内障发生过程中血清中循环的特异性自身抗体。
用链脲佐菌素(STZ;55 mg/kg体重)诱导雄性Wistar/NIN糖尿病大鼠(2 - 3月龄),并将对照非糖尿病大鼠用于本研究。在注射后第0天以及直至第8周每隔两周对两组大鼠的血糖、糖化血红蛋白和体重进行评估。还估计了其他生化参数,如晶状体蛋白中非蛋白质巯基(-SH)基团的水平和γ-谷氨酰转肽酶(γ-GT)的活性。通过采用基于数字的图像分析和荧光分光光度法测量完整晶状体以及晶状体匀浆中晚期糖基化终产物(AGE)样荧光团来监测白内障进展。同样,使用针对β-糖化、γ-糖化、β-和γ-晶状体蛋白的多克隆抗体,通过非竞争性ELISA测定晶状体中各自免疫原的浓度,并通过抗体捕获试验测定其各自的循环抗体。通过蛋白质印迹技术评估白内障发生过程中糖化晶状体蛋白(可溶性和不溶性部分)的情况。
STZ诱导的糖尿病大鼠表现出典型的糖尿病症状(高血糖、水和食物摄入量增加但体重未增加)。对总晶状体蛋白的生化分析显示非蛋白质-SH基团水平显著降低(p = <0.001)。与对照组相比,发现糖尿病大鼠晶状体γ-GT的活性未改变。对完整晶状体的数字分析表明,在白内障发生过程中与AGE样荧光团的形成呈正相关(r(2)=0.888)。在糖尿病动物的总晶状体匀浆中,在白内障发生过程中AGE样荧光团水平也观察到类似趋势。通过非竞争性ELISA分析大鼠晶状体(可溶性和不溶性部分)中β-和γ-糖化晶状体蛋白的浓度。与对照组相比,发现到第8周结束时β-和γ-糖化晶状体蛋白的浓度增加。同时,从第2周起在糖尿病大鼠血清中也检测到晶状体蛋白特异性(β-和γ-糖化晶状体蛋白)自身抗体。蛋白质印迹分析表明在不溶性部分中糖化晶状体蛋白(β-和γ-晶状体蛋白)的形成增加。
在白内障发生过程中观察到以下情况:(1)完整晶状体中AGE样荧光团的形成增加;(2)到第8周结束时大鼠晶状体(不溶性部分)中β-和γ-糖化晶状体蛋白水平增加;(3)这些糖化晶状体蛋白释放到外周循环中导致产生针对β-和γ-糖化晶状体蛋白的自身抗体,在实验大鼠诱导糖尿病状态后最早在第2周即可检测到。
