巨噬细胞炎症蛋白-1ɑ拮抗剂联合硼替佐米通过抑制Erk1/2/Bax促进骨髓瘤骨病成骨的作用

doi:10.3969/j.issn.1006⁃5725.2021.12.004

实用医学杂志 ›› 2021, Vol. 37 ›› Issue (12): 1529-1533.doi: 10.3969/j.issn.1006⁃5725.2021.12.004

巨噬细胞炎症蛋白-1ɑ拮抗剂联合硼替佐米通过抑制Erk1/2/Bax促进骨髓瘤骨病成骨的作用

陈卫琼，蒋芳，王姗姗，黄勃，屈付君，黄林，王晓桃

桂林医学院第二附属医院（广西桂林 541100）

出版日期:2021-06-25 发布日期:2021-06-25
通讯作者: 王晓桃 E⁃mail：wxttjl@126.com
基金资助:
国家自然科学基金（编号：82060044）；广西自然科学基金（编号：2020aXNSFAA159018）

MIP⁃1ɑ antagonist combined with bortezomib promotes osteoblasts in myeloma bone disease by inhibiting Erk1/2/Bax

CHEN Weiqiong，JIANG Fang，WANG Shanshan，HUANG Bo，QU Fujun，HUANG Lin，WANG Xiaotao.

The Second Affiliated Hospital of Guilin Medical College，Guilin 541100，China

Online:2021-06-25 Published:2021-06-25
Contact: WANG Xiaotao E⁃mail：wxttjl@126.com

摘要/Abstract

摘要：

目的探讨巨噬细胞炎症蛋白⁃1α（MIP⁃1α）拮抗剂联合硼替佐米通过抑制 Erk1/2/Bax 促进骨髓瘤骨病（myeloma bone disease，MBD）成骨作用。方法采用皮下注射骨髓瘤细胞株方法构建 MBD 小鼠模型，按药物给予分为对照组、硼替佐米（Bor）组、Bx471（MIP⁃1α拮抗剂）组、硼替佐米（Bor）联合 Bx471 （MIP⁃1α拮抗剂）组；ELISA 检测 MIP⁃1α、SOST、IL⁃6、BALP、RANKL、OPG 水平，Western blot 检测 Erk、Bax、 Caspase 3、Caspase 9 表达水平，X 线评估骨质破坏程度。结果 X 线显示荷瘤小鼠（对照组）出现病理性骨折，Bor 组、Bx471 组及 Bor 联合 Bx471 组骨质破坏程度低于对照组。对照组的 MIP⁃1α、SOST、RANKL、IL⁃6 水平高于 Bor 组及 Bx471 组（P < 0.05），明显高于 Bor 联合 Bx471 组（P < 0.001），而 OPG、BALP 的表达明显低于 Bor 联合 Bx471 组（P < 0.001）。对照组的 Erkl/2、Bax、Caspase 3、Caspase 9 蛋白表达高于 Bor 组及 Bx471 组（P < 0.05），且明显高于 Bor 联合 Bx471 组（P < 0.001）。结论 MIP⁃1ɑ拮抗剂联合硼替佐米可能抑制Erk1/2/Bax 信号通路促进MBD 成骨作用。

关键词:

MIP?1ɑ拮抗剂, 硼替佐米, 骨髓瘤骨病, Erk1/2/Bax ,

Abstract:

Objective To investigate the role of MIP⁃1ɑ antagonist combined with bortezomib in the facili⁃ tation of osteoblasts in myeloma bone disease（MBD）by inhibiting Erk1/2/Bax. Methods A MBD mouse model was constructed by subcutaneous injection of myeloma cell lines. The mice were divided into four groups ：the control group，Bortezomib（Bor）group，MIP ⁃ 1ɑ antagonist（Bx471）group，Bor combined with Bx471（Bor + Bx471）group. Enzyme linked immunosorbent assay（ELISA）was used to detect the expression levels of MIP ⁃1ɑ， SOST，IL⁃6，BALP，RANKL，and OPG and Western blotting the expression levels of Erk，Bax，Caspase 3， Caspase 9，and X⁃ray to assess the degree of bone destruction. Results X⁃ray tests showed that the tumor⁃bearing mice in the control group had pathological fractures. As compared with the control group，the bone destructions in the other three groups were at a lower level. In contrast，the levels of MIP⁃1α，SOST，RANKL，and IL⁃6 in the control group were significantly higher than in Bor group and Bx471 group（P < 0.05），especially than in Bor+ Bx471 group（P < 0.001），while the expressions of OPG and BALP were significantly lower than in the Bor com⁃ bined with Bx471 group（P < 0.001）. The protein expressions of Erkl/2，Bax，Caspase 3，Caspase 9 in the control group were higher than in Bor group and Bx471 group（P < 0.05），especially than in Bor + Bx471 group（P < 0.001）. Conclusions MIP⁃1ɑ antagonists combined with bortezomib may inhibit the Erk1/2/Bax signaling pathway and then promote MBD osteoblasts.

Key words:

MIP?1ɑ antagonist, bortezomib, myeloma bone disease, myeloma bone disease, Erk1/2/Bax

陈卫琼, 蒋芳, 王姗姗, 黄勃, 屈付君, 黄林, 王晓桃 .

巨噬细胞炎症蛋白-1ɑ拮抗剂联合硼替佐米通过抑制Erk1/2/Bax促进骨髓瘤骨病成骨的作用 [J]. 实用医学杂志, 2021, 37(12): 1529-1533.

CHEN Weiqiong, JIANG Fang, WANG Shanshan, HUANG Bo, QU Fujun, HUANG Lin, WANG Xiaotao. .

MIP⁃1ɑ antagonist combined with bortezomib promotes osteoblasts in myeloma bone disease by inhibiting Erk1/2/Bax [J]. The Journal of Practical Medicine, 2021, 37(12): 1529-1533.

巨噬细胞炎症蛋白-1ɑ拮抗剂联合硼替佐米通过抑制Erk1/2/Bax促进骨髓瘤骨病成骨的作用

MIP⁃1ɑ antagonist combined with bortezomib promotes osteoblasts in myeloma bone disease by inhibiting Erk1/2/Bax

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 0

编辑推荐

Metrics

本文评价