孢子油能增强环磷酰胺抑制程序性死亡-1的效果,延长H22肿瘤小鼠的存活时间。

Jiang Zhaojian, Cai Hongfei, Yuan Cheng, Cao Lin, X U Wendong, Han Yaming, Zhang Qin, L I Jing, Wang Qin, Liu Juyan
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引用次数: 0

摘要

研究目的研究灵芝孢子油(GLSO)对环磷酰胺(CTX)治疗H22肿瘤小鼠肿瘤生长和生存的影响,并探讨其潜在机制:方法:应用异种移植H22肝细胞癌小鼠模型研究GLSO对肿瘤生长和动物生存的影响,并采用Kaplan-Meier生存分析法分析动物的生存期。血浆生化检查用于检测丙氨酸氨基转移酶(ALT)、天冬氨酸氨基转移酶(AST)、尿素(UREA)和肌酐(CRE)的水平。对程序性死亡-1(PD-1)、程序性死亡配体1(PD-L1)、Janus激酶2(JAK2)、磷酸化信号转导和转录激活因子3(p-STAT3)以及信号转导和转录激活因子3(STAT3)的表达进行了蛋白质印迹分析:结果:GLSO提高了CTX的抗肿瘤效果,延长了接受CTX治疗的H22肿瘤小鼠的生存期。同时,GLSO能提高胸腺指数,对动物肝功能无明显毒性。GLSO 还能降低接受 CTX 治疗的 H22 肿瘤小鼠体内的脲尿酸水平。此外,GLSO还能抑制脾脏中PD-1的表达,这与JAK2的表达和STAT3的磷酸化无关。然而,GLSO并不影响肿瘤组织中PD-L1、JAK2和p-STAT3的表达:结论:GLSO 可增强 CTX 的抗肿瘤作用,延长 H22 肿瘤小鼠的寿命,其潜在机制可能与胸腺功能的改善作用和抑制 PD-1 在脾脏的表达有关。此外,这些研究结果还表明,在肝细胞癌的临床化疗中,GLSO与CTX联用可延长患者的生存期。
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Spore Oil enhances the effect of cyclophosphamide inhibiting programmed death-1 and prolongs the survival of H22 tumor-bearing mice.

Objective: To investigate the effect of Ganoderma Lucidum Spore Oil (GLSO) on the tumor growth and survival of H22 tumor-bearing mice treated with cyclophosphamide (CTX), and explore the underlying mechanism.

Methods: Allograft H22 hepatocellular carcinoma mouse model was applied to investigate the effect of GLSO on the tumor growth and survival of animals, and Kaplan-Meier survival analysis was used to analyze the life span. Plasma biochemical examination was used to determine the levels of alanine aminotransferase (ALT), aspartate aminotransferase (AST), urea (UREA) and creatinine (CRE). Western blot analysis was performed to detect Programmed Death-1 (PD-1), Programmed Death Ligand 1 (PD-L1), Janus Kinase 2 (JAK2), phosphorylated Signal Transducer and Activator of Transcription 3 (p-STAT3), and Signal Transducer and Activator of Transcription 3 (STAT3) expression.

Results: GLSO increased the anti-tumor effect of CTX and prolonged the survival of H22 tumor-bearing mice treated with CTX. Meanwhile, GLSO increased the thymus index and showed no obvious toxicity to liver functions of animals. GLSO also decreased the level of UREA in H22 tumor-bearing mice treated with CTX. Furthermore, GLSO could inhibit the expression of PD-1 in spleen, which was independent of JAK2 expression and STAT3 phosphorylation. However, GLSO did not affect the expression of PD-L1, JAK2, and p-STAT3 in tumor tissue.

Conclusion: GLSO could strengthen the anti-tumor effect of CTX and prolong the life span of H22 tumor-bearing mice, while the underlying mechanism might be relevant to the amelioration effect of thymus function and inhibition of PD-1 expression in spleen. Furthermore, these findings implied the promising role of GLSO in combination with CTX to extend the survival of patients in clinical chemotherapy of hepatocellular carcinoma.

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