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Testicular toxicity and sperm quality following copper exposure in Wistar albino rats: ameliorative potentials of L-carnitine

机译:Wistar Albino大鼠铜暴露后睾丸毒性和精子质量:L-肉碱的改复潜力

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摘要

Copper is a persistent toxic and bio-accumulative heavy metal of global concern. Continuous exposure of copper compounds of different origin is the most common form of copper poisoning and in turn adversely altering testis morphology and function and affecting sperm quality. L-carnitine has a vital role in the spermatogenesis, physiology of sperm, sperm production and quality. This study was designed to examine whether the detrimental effects of long-term copper consumption on sperm quality and testis function of Wistar albino rat could be prevented by L-carnitine therapy. The parameters included were sperm quality (concentration, viability, motility, and morphology), histopathology, serum aspartate aminotransferase (AST), serum alanine aminotransferase (ALT), serum urea, serum creatinine, serum testosterone and testis antioxidant enzyme levels (superoxide dismutase and glutathione-S-transferase), and biomarkers of oxidative stress (lipid peroxidation and expression of heat shock protein 70 in testis). Three-month-old male Wistar rats (n = 30) were divided into six groups as group 1 (G1, 0.9% saline control), group 2 (G2, CuSO4 200 mg/kg dissolved in 0.9% saline water), groups 3 and 4 (G3 and G4, L-carnitine 50 and 100 mg/kg dissolved in 0.9% saline water, respectively), and groups 5 and 6 (G5 and G6, CuSO4 200 mg/kg plus L-carnitine, 50 and 100 mg/kg dissolved in 0.9% saline water, respectively). Doses of copper (200 mg/kg) and L-carnitine (50 and 100 mg/kg) alone and in combinations along with untreated control were administered orally for 30 days. The following morphological, physiological, and biochemical alterations were observed due to chronic exposure of copper (200 mg/kg) to rats in comparison with the untreated control: (1) generation of oxidative stress through rise in testis lipid peroxidation (12.21 vs 3.5 nmol MDA equivalents/mg protein) and upregulation of heat shock protein (overexpression of HSP70 in testis), (2) liver and kidney dysfunction [elevation in serumALT (81.65 vs 48.08 IU/L), AST (156.82 vs 88.25 IU/L), ALP (230.54 vs 148.16 IU/L), urea (12.65 vs 7.45 mmol/L), and creatinine (80.61 vs 48.25 mu mol/L) levels], (3) significant decrease in body (99.64 vs 106.09 g) and organ weights (liver-3.48 vs 4.99 g; kidney-429.29 vs 474.78 mg; testes-0.58 vs 0.96 g), (4) imbalance in hormonal and antioxidant enzyme concentrations [significant decline in serum testosterone (0.778 vs 3.226 ng/mL), superoxide dismutase (3.07 vs 8.55 mu mol/mg protein), and glutathione-S-transferase (59.28 vs 115.58 nmol/mg protein) levels], (5) severe alterations in the testis histomorphology [sloughed cells (90.65%, score 4 vs 15.65%, score 1), vacuolization (85.95%, score 4 vs 11.45%, score 1), cellular debris along with degenerative characteristics, accentuated germ cell depletion in the seminiferous epithelium, severe damage of spermatogonia and Sertoli cells (73.56%, score 3 vs 0%, score 1)], (6) suppression of spermatogenic process [hypospermatogenesis (low Jhonsen testicular biopsy score 4 vs 9.5), decrease in tubules size (283.75 vs 321.25 mu m in diameter), and no. of germ cells (81.8 vs 148.7/100 tubules), Leydig cells (5.2 vs 36.65/100 tubules), and Sertoli cells (8.1 vs 13.5/100 tubules)], (7) sperm transit time was shorter in caput and cauda and ensued in incomplete spermatogenic process and formation of immature sperm leading to infertility, (8) sperm quality was affected significantly [decreased daily sperm production (13.21 vs 26.9 x 10(6) sperms/mL), sperm count (96.12 vs 154.
机译:铜是全球关注的持续有毒和生物累积重金属。不同起源的铜化合物的连续暴露是最常见的铜中毒形式,反过来不利地改变睾丸形态和功能并影响精子质量。 L-肉碱在精子发生,精子,精子生产和质量的生理学中具有重要作用。该研究旨在检测长期铜消耗对Wistar Albino大鼠的精子质量和睾丸功能的不利影响是否可以通过L-肉碱治疗预防。包括的参数是精子质量(浓度,活力,运动和形态),组织病理学,血清天冬氨酸氨基转移酶(AST),血清丙氨酸氨基转移酶(ALT),血清尿素,血清肌酐,血清睾酮和睾丸抗氧化酶水平(超氧化物歧化酶和谷胱甘肽-S-转移酶和氧化应激的生物标志物(睾丸中的脂质过氧化和热休克蛋白70的表达)。将三个月的雄性Wistar大鼠(n = 30)分为六组,为第1组(G1,0.9%盐水管),第2组(G2,Cuso4 200 mg / kg溶解在0.9%盐水中),3组和4(G3和G4,L-肉碱50和100mg / kg分别溶解在0.9%盐水中)和组5和6(G5和G6,CusO4 200 mg / kg加1-Carnitine,50和100mg / kg分别溶于0.9%盐水中)。单独使用单独的铜(200mg / kg)和1-丙氨酸(50和100mg / kg)以及未处理对照的剂量,口服给予30天。与未处理对照的慢性暴露于铜(200mg / kg)的慢性暴露于大鼠的慢性暴露,观察到以下形态,生理和生化改变:(1)通过睾丸脂质过氧化的升高产生氧化胁迫(12.21 vs 3.5 Nmol MDA当量/ mg蛋白质)和热休克蛋白的上调(睾丸中的HSP70过度表达),(2)肝肾功能障碍[血清中的升高(81.65 Vs 48.08 IU / L),AST(156.82 VS 88.25 IU / L), ALP(230.54 vs 148.16 IU / L),尿素(12.65 Vs 7.45mmol / L),肌酐(80.61 vs 48.25 mol / l)水平],(3)体内的显着降低(99.64 vs 106.09g)和器官重量(肝脏-3.48 vs 4.99 g;肾脏-229.29与474.78 mg;睾丸-0.58 vs 0.96g),(4)激素和抗氧化酶浓度的不平衡[血清睾酮的显着下降(0.778 Vs 3.226ng / ml),超氧化物歧化酶(3.07 Vs 8.55 mo mol / mg蛋白)和谷胱甘肽-S-转移酶(59.28 vs 115.58 nmol / mg蛋白)水平] ,(5)睾丸组织形态学的严重改变[脱落细胞(90.65%,得分4与15.65%,得分1),真空化(85.95%,得分4与11.45%,得分1),细胞碎片以及退行性特征,强调生殖细胞耗尽在嗜血体上皮,精子损伤的严重损伤和血清细胞(73.56%,得分3 vs 0%,得分1)],(6)抑制精子生成过程[低血量发育(低jhonsen睾丸活检4 Vs 9.5),小管尺寸减少(直径为283.75毫米321.25μm),没有。胚芽细胞(81.8 Vs 148.7 / 100小管),Leydig细胞(5.2 Vs 36.65 / 100小管)和Sertoli细胞(8.1 vs 13.5 / 100小管),(7)精子转运时间较短,并在毛滩较短,并随后短在不完全的精子遗传学过程中,未经成分的形成导致不孕症,(8)精子质量受到显着影响[每日精子产生降低(13.21 vs 26.9×10(6)个子/ ml),精子计数(96.12 Vs 154。

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