Therapeutic effect and mechanisms of Changyanning Tablets on colorectal adenoma-carcinoma model rats

ZHANG Kaixuan; YANG Yang; FU Zhiwen; JIA Shengjuan; WEI Wei

doi:10.16025/j.1674-1307.2024.09.002

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Therapeutic effect and mechanisms of Changyanning Tablets on colorectal adenoma-carcinoma model rats

更新时间：2024-10-14

- Therapeutic effect and mechanisms of Changyanning Tablets on colorectal adenoma-carcinoma model rats
- Beijing Journal of Traditional Chinese Medicine Vol. 43, Issue 9, Pages: 964-972(2024)
- 作者机构：
  
  1.中国中医科学院望京医院脾胃病科，北京 100102
  2.江西康恩贝中药有限公司，上饶 334499
- 作者简介：
- 基金信息：
- DOI：10.16025/j.1674-1307.2024.09.002
  CLC：
- Published：25 September 2024，
  
  Received：19 June 2024，
- 稿件说明：
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张凯轩，杨洋，付志文，等.肠炎宁片对结直肠腺瘤-癌模型大鼠的治疗作用及机制［J］.北京中医药，2024，43（9）：964-972.

ZHANG Kaixuan,YANG Yang,FU Zhiwen,et al.Therapeutic effect and mechanisms of Changyanning Tablets on colorectal adenoma-carcinoma model rats[J]. Beijing Journal of Traditional Chinese Medicine,2024,43(09):964-972.
张凯轩，杨洋，付志文，等.肠炎宁片对结直肠腺瘤-癌模型大鼠的治疗作用及机制［J］.北京中医药，2024，43（9）：964-972. DOI： 10.16025/j.1674-1307.2024.09.002.

ZHANG Kaixuan,YANG Yang,FU Zhiwen,et al.Therapeutic effect and mechanisms of Changyanning Tablets on colorectal adenoma-carcinoma model rats[J]. Beijing Journal of Traditional Chinese Medicine,2024,43(09):964-972. DOI： 10.16025/j.1674-1307.2024.09.002.

摘要

目的

观察肠炎宁片对结直肠腺瘤-癌（CRA-CRC）模型大鼠的治疗作用，探讨其可能的作用机制。

方法

随机取6只大鼠作为正常组（Normal组），其余30只大鼠制备CRA-CRC模型，予1，2-二甲基肼二盐酸盐（1，2-DMH）60 mg/kg腹腔注射，1次/周，持续15周。第7周，采用随机区组设计将模型大鼠分为模型组（Model组）、黄连素组（HLS组）、肠炎宁片低剂量组（L-CYN组）、肠炎宁片中剂量组（M-CYN组）、肠炎宁片高剂量组（H-CYN组），每组6只。HLS组给予0.027 g/kg黄连素灌胃，L-CYN组、M-CYN组、H-CYN组分别给予0.3、0.6、1.2 g/kg肠炎宁片灌胃，Normal组、Model组给予等量蒸馏水灌胃。均1次/d，持续8周。对比各组一般情况、体质量、腹腔解剖结构及肠道肿瘤发生情况、肠道肿瘤组织病理变化、结直肠组织中血管内皮生长因子（VEGF）蛋白表达和凋亡相关蛋白Cleaved Caspase-3表达。

结果

造模第15周，与Normal组比较，Model组体质量低（

0.05）；与Model组比较，HLS组、L-CYN组、M-CYN组、H-CYN组体质量差异无统计学意义（

0.05）。Model组大鼠腹腔有大量腹水。各组大鼠腹腔均未见明显脏器异常，肉眼观察未见肿瘤脏器转移。与Normal组比较，Model组大鼠结直肠长度短（P

0.05），肿瘤数量多（

0.01）；与Model组比较，H-CYN组大鼠结直肠长度长（

0.05），HLS组、H-CYN组、M-CYN组大鼠肿瘤

数量少（

0.05），H-CYN组有1只大鼠肉眼未观察到肿瘤。与Normal组比较，Model组大鼠肿瘤大（

0.01）；与Model组比较，HLS组、H-CYN组、M-CYN组大鼠肿瘤小（

0.01，

0.05）。Model组结肠腺体和细胞数量明显增加，细胞间有大量炎症细胞浸润，细胞排列密集，可见大小与形态显著变化的肿瘤细胞，含有大而深染的细胞核，核分裂现象多，局灶腺体可见中-重度异型增生、高级别上皮内瘤变、局灶原位癌形成。L-CYN组杯状细胞消失，细胞增生，排列紧密，有明显的核分裂，可见许多细小核仁。HLS组和M-CYN组病理结果相仿，可见淋巴滤泡增生、腺体修复样改变、隐窝脓肿、固有腺体局灶减少。H-CYN组腺体排列较整齐，局灶炎症细胞浸润、糜烂、固有腺体局灶减少，核分裂现象偶见。Model组大鼠腺癌发生率为50%，管状腺瘤发生率为33.3%，另1只大鼠为重度异型增生，所有大鼠均造模成功。L-CYN组大鼠肠道肿瘤组织病理变化改善不明显，HLS组、M-CYN组、H-CYN组肠道肿瘤组织病变程度减轻，其中H-CYN组效果最明显。与Model组比较，L-CYN组大鼠VEGF蛋白表达低，但差异无统计学意义（

0.05），HLS组、M-CYN组、H-CYN组大鼠VEGF蛋白表达低（

0.05）。与Normal组比较，Model组大鼠结直肠组织中Cleaved Caspase-3蛋白表达低（

0.05）。与Model组比较，各中药治疗组和HLS结直肠组织中Cleaved Caspase-3蛋白表达高（

0.05，

0.01）。

结论

肠炎宁片可以改善CRA-CRC模型大鼠临床症状及结直肠黏膜病理变化，其作用机制可能与降低VEGF表达并促进Cleaved Caspase-3表达有关。

Abstract

Objective

To observe the therapeutic effect of Changyanning Tablets on colorectal adenoma-carcinoma （CRA-CRC） model rats and explore its possible mechanisms.

Methods

Six rats were randomly assigned to the normal group （Normal）. The remaining rats were intraperitoneally injected with 1，2-dimethylhydrazine （DMH） at 60 mg/kg once a week for 15 weeks to establish the CRA-CRC model. In the 7th week， the model rats were randomly divided into five groups according to a randomized block design： a model group （Model）， a berberine group （HLS）， a low dose group of Changyanning Tablets （L-CYN）， a medium dose group of Changyanning Tablets （M-CYN）， and a high dose group of Changyanning Tablets （H-CYN）， with 6 rats in each group. From the 7th week of modeling， the HLS group was given berberine at 0.027 g/kg by gavage， while the L-CYN， M-CYN， and H-CYN groups were given Changyanning Tablets at 0.3， 0.6， and 1.2 g/kg by gavage， respectively. The Normal and Model groups were given distilled water by gavage. The above drug treatments were performed once daily for 8 weeks. General conditions， body weight， abdominal anatomical structure， incidence of intestinal tumors， pathological changes in intestinal tumor tissues， vascular endothelial growth factor （VEGF） protein expression in colorectal tissues， and cleaved Caspase-3 expression were compared among the groups.

Results

By the 15th week of modeling， compared with the Normal group， the Model group had a lower body weight （

0.05）. No significant difference in body weight was observed in the HLS， L-CYN， M-CYN， and H-CYN groups compared with the Model group （

0.05）. The Model group showed a large amount of ascites. No obvious organ abnormalities or tumor metastasis were observed in the abdominal cavity of rats in any group. Compared with the Normal group， the Model group had a shorter colorectal length （

0.05） and a higher number of tumors （

0.01）. Compared with the results in the Model group， the colorectal length in the H-CYN group was longer （

0.05）， and the number of tumors was lower in the HLS， H-CYN， and M-CYN groups （

0.05）， with one rat in the H-CYN group showing no visible tumors. Tumor size was larger in the Model group than in the Normal group （

0.01）， and smaller in the HLS， H-CYN， and M-CYN groups （

0.01）. The Model group showed significant increases in gland and cell numbers in the colon， extensive inflammatory cell infiltration between cells， dense cell arrangement， and significant changes in tumor cell size and morphology， including large and deeply stained nuclei， frequent nuclear division， and focal glandular severe atypical hyperplasia， high-grade intraepithelial neoplasia， and focal in situ carcinoma formation. In the L-CYN group， goblet cells disappeared， cells proliferated and were closely arranged

， with obvious nuclear division and numerous small nucleoli. The HLS and M-CYN groups had similar pathological results， including lymph follicle hyperplasia， glandular repair-like changes， crypt abscesses， and focal reduction of inherent glands. The H-CYN group had more organized gland arrangement， focal inflammatory cell infiltration， erosion， and focal reduction of inherent glands， with occasional nuclear division. The Model group had an incidence of adenocarcinoma of 50% and tubular adenoma of 33.3% （with mild and moderate atypical hyperplasia）， and one rat with severe atypical hyperplasia. All rats were successfully modeled. The pathological changes in intestinal tumor tissues in the L-CYN group were not significantly improved， whereas the HLS， M-CYN， and H-CYN groups showed reduced tumor tissue lesions， with the H-CYN group showing the most significant effect. Compared with the results in the Model group， VEGF protein expression was lower in the L-CYN group， though not statistically significant （

0.05）， and significantly lower in the HLS， M-CYN， and H-CYN groups （

0.05）. Cleaved Caspase-3 protein expression was lower in the colorectal tissues of the Model group than that in the Normal group （

0.05）. Cleaved Caspase-3 protein expression was higher in the colorectal tissues of the Chinese medicine treatment groups and the HLS group than that in the Model group （

0.05，

0.01）.

Conclusion

Changyanning Tablets can improve clinical symptoms and pathological changes in the colorectal mucosa of CRA-CRC model rats， and its mechanism may be related to the negative regulation of VEGF expression and the promotion of cleaved Caspase-3 expression.

关键词

肠炎宁片结直肠癌结直肠腺瘤癌前病变血管内皮生长因子活性半胱氨酸天冬氨酸蛋白水解酶3

Keywords

Changyanning Tabletscolorectal cancercolorectal adenomasprecancerous lesionsVEGFcleaved Caspase-3

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