甘草酸二胺对CRP/TGF-β介导的慢性肝炎性纤维化的作用研究

目的探讨甘草酸二胺对C反应蛋白(CRP)、转化生长因子β(TGF-β)介导的慢性肝炎性纤维化的作用研究。方法 2021年9月至12月, 选取50只大鼠[8周龄, 体质量(200±20)g/只], 分为对照组、模型组、高剂量组、中剂量组、低剂量组, 每组10只, 采用刀豆蛋白A建立慢性肝炎纤维化模型, 采用高、中、低剂量甘草酸二胺灌胃干预, 而对照组、模型组给予等剂量生理盐水。比较各组大鼠肝脏病理改变、血清C反应蛋白(CRP)、谷丙转氨酶(ALT)、谷草转氨酶(AST)水平及透明质酸(HA)、层粘连蛋白(LN)、I型胶原蛋白(PC Ⅰ)、Ⅲ型胶原蛋白(PC Ⅲ)等纤维化相关指标含量;采用聚合酶链反应(PCR)检测肝组织CRP、TGF-β、LN、PC Ⅰ、PC Ⅲ mRNA表达;Western blot法检测肝组织CRP、TGF-β、LN、PC Ⅰ、PC Ⅲ蛋白表达情况。组间比较采用t检验, 多组间比较采用单因素方差分析。结果与对照组相比, 模型组CRP[(7.34±1.19)mg/L比(121.98±1.37)mg/L]、ALT[(48.32±16.92)U/L比(169.31±20.31)U/L]、AST[(29.28±18.12)U/L比(163.08±25.97)U/L]、HA[(7.98±1.23)mg/L比(17.39±1.39)mg/L]、LN[(73.20±11.08)μg/L比(119.34±14.98)μg/L]、PC Ⅰ[(8.09±1.57)μg/L比(27.46±2.05)μg/L]、PC Ⅲ[(9.07±1.69)μg/L比(29.91±2.17)μg/L]水平均显著升高(均P<0.05);与模型组比较, 随剂量增加, 低剂量组、中剂量组、高剂量组CRP[(87.20±1.29)mg/L比(53.19±1.23)mg/L比(18.29±1.20)mg/L]、ALT[(112.87±19.28)U/L比(87.29±18.78)U/L比(57.92±17.38)U/L]、AST[(139.98±23.09)U/L比(102.35±21.34)U/L比(78.98±19.87)U/L]、HA[(14.27±1.28)mg/L比(10.31±1.27)mg/L比(8.38±1.25)mg/L]、LN[(102.47±13.37)μg/L比(82.37±12.84)μg/L比(78.39±12.06)μg/L]、PC Ⅰ[(22.98±1.82)μg/L比(16.62±1.72)μg/L比(10.35±1.68)μg/L]、PC Ⅲ[(23.23±1.79)μg/L比(17.45±1.78)μg/L比(12.57±1.72)μg/L]水平明显降低, 差异均有统计学意义(均P<0.05);与对照组相比, 模型组CRP[(0.92±0.23)比(2.98±0.32), (0.87±0.08)比(2.94±0.21)]、TGF-β[(1.19±0.17)比(3.29±0.29), (1.09±0.07)比(3.02±0.23)]、LN[(0.93±0.18)比(3.91±0.38), (1.18±0.10)比(3.45±0.26)]、PC Ⅰ[(1.02±0.22)比(4.32±0.32), (1.08±0.08)比(3.96±0.28)]、PC Ⅲ[(1.23±0.19)比(4.23±0.29), (1.13±0.10)比(3.32±0.23)]mRNA及蛋白表达均显著升高(均P<0.05);与模型组比较, 随剂量增加低剂量组、中剂量组、高剂量组CRP[(2.21±0.28)比(1.97±0.30)比(1.39±0.26), (1.96±0.18)比(1.54±0.14)比(1.18±0.09)]、TGF-β[(2.94±0.24)比(2.09±0.27)比(1.49±0.20), (2.18±0.21)比(1.86±0.19)比(1.28±0.14)]、LN[(3.09±0.30)比(2.39±0.26)比(1.52±0.25), (2.46±0.24)比(1.87±0.20)比(1.37±0.16)]、PC Ⅰ[(2.93±0.28)比(1.82±0.24)比(1.28±0.20), (2.08±0.28)比(1.76±0.24)比(1.29±0.13)]、PC Ⅲ[(3.21±0.25)比(2.19±0.28)比(1.47±0.24), (2.87±0.20)比(2.09±0.19)比(1.21±0.11)]mRNA及蛋白表达明显降低, 差异均有统计学意义(均P<0.05)。结论高剂量甘草酸二胺可缓解肝纤维化, 抑制PCR、TGF-β表达是介导这一改善作用的可能分子机制。

Transforming growth factor-β1 gene polymorphisms are associated with progression of liver fibrosis in Caucasians with chronic hepatitis C infection

AIM: Considerable attention is focused on polymorphisms in the gene encoding transforming growth factor-pi (TGF-β1), a multifunctional cytokine that is in turn a potent growth inhibitor involved in wound healing and differentiation. In humans, it promotes the pathogenesis of organ fibrosis, atherosclerosis, cancer, autoimmune and inflammatory diseases, keloid disease, and hypertrophic scarring. For this reason, much emphasis has been placed on studies elucidating the impact of TGF-β1 and its gene variations for the susceptibility and pathogenesis of these diseases. Unfortunately, some studies have serious limitations. METHODS: We have recently described a high-throughput method for investigation the Arg25Pro polymorphism of human TGF-β1 gene and showed that the frequency of the Pro25 allele is significantly associated with hepatic fibrogenesis. In this report, we describe two novel LightCyder (LC) techniques that facilitate the examination of the two other known alterations in the coding region of TGF-β1. We investigated whether these polymorphisms contribute to hepatitis-induced progression of fibrogenesis in Chinese and Caucasians. RESULTS: In the Chinese ancestry, the gene polymorphisms at codons 25 and 263 were not found and the genetic variant at codon 10 is unlikely to confer susceptibility to hepatic fibrosis. Contrarily, in Caucasians TGF-β1 allelic variations are more frequent and the presence of prolines either in codon 25 or 10 is associated with the interindividual variability in developing more severe fibrosis during chronic hepatitis C infection. CONCLUSION: In summary, these results confirm the hypothesis that TGF-β1 polymorphisms are associated with fibrosis progression in Caucasians chronically infected with hepatitis C.