共刺激分子B7⁃H3在急性髓系白血病中的表达及生物学意义

doi:10.7655/NYDXBNS20180112

首页 > 过刊浏览>2018年第卷第1期 >54-58. DOI:10.7655/NYDXBNS20180112

共刺激分子B7⁃H3在急性髓系白血病中的表达及生物学意义
DOI:
                        10.7655/NYDXBNS20180112
                    
作者:
                        
                        
                    
作者单位:
作者简介:
通讯作者:
中图分类号:
基金项目:国家自然科学基金（81270652）

Expression of costimulatory molecule B7⁃H3 on human acute myeloid leukemia and its biological significance

Author:

Affiliation:

Fund Project:

摘要

图/表

访问统计

参考文献

相似文献

引证文献

资源附件

文章评论

摘要:

目的：检测共刺激分子B7-H3在初诊急性髓系白血病（human acute myeloid leukemia，AML）患者中的表达，探讨其临床意义。方法：应用流式细胞术（FCM）检测66例初诊AML患者原始幼稚细胞群上B7-H3分子膜蛋白的表达，RT-PCR技术检测B7-H3 mRNA产物的表达。分析B7-H3分子的表达与AML患者发病时年龄、性别、初诊时外周血白细胞计数以及染色体之间的关系，评估B7-H3分子的表达与患者的无进展生存期（progression-free survival，PFS）和总体生存期（overall survival，OS）之间的关系。结果：正常对照组B7-H3分子表达阴性。共刺激分子B7-H3在66例初诊AML患者中阳性表达率为42%（28/66）。在不同性别、年龄和白细胞分组中，B7-H3阳性率表达无统计学差异（P=0.924，0.541，0.310）；预后差染色体变异组的B7-H3分子的阳性表达率明显高于预后好及中等预后组（P＜0.001）。B7-H3分子阳性组患者的PFS（7.4个月vs. 15.2个月）及OS（9.8个月vs. 17.8个月）均明显低于阴性组患者（P＜0.05）。此外，在AML-M2亚型中，预后差染色体变异组B7-H3分子的表达明显高于预后好及中等预后组（30.05% ± 23.10% vs. 10.08% ± 7.07%，P＜0.001），B7-H3与骨髓白血病细胞CD34存在共表达，并且CD34阳性组的B7-H3分子表达明显高于CD34阴性组（20.90% ± 19.70% vs. 9.63% ± 7.21%，P=0.034）。结论：共刺激分子B7-H3的表达对于AML患者的病情进展有一定影响，B7-H3分子表达阳性的患者预后更差。B7-H3对AML的预后判断和指导临床治疗具有重要意义。

Abstract:

Objective：To analyze the expression of costimulatory molecule B7-H3 in patients with acute myeloid leukemia（AML），and explore the clinical significance of the expression of B7-H3. Methods：The expression of B7-H3 protein was detected by flow cytometry（FCM）and the expression of B7-H3 mRNA was detected by RT-PCR. We analyzed the relationship between the expression of B7-H3 and some clinical factors. We evaluated the progression-free survival（PFS）and overall survival（OS）between the B7-H3 positive group and the B7-H3 negative group. Results：The results demonstrated that B7-H3 was weakly expressed on bone marrow of AML patients，and RT-PCR also detected mRNA of B7-H3. No B7-H3 positive cells were detected in the normal human bone marrow. B7-H3 was detected in 28 of the 66 cases（42％）. However，among 66 AML cases，no significantly higher frequency of B7-H3 positive cases was found in the male or female group（P=0.924）. Neither was observed between patients who were older than 60 years and those less than 60 years（P=0.541）. The B7-H3 positive expression was of no significant within the higher WBC subset（≥ 30×109/L）（P=0.310）. There was significant differences between favorable karyotype subset and unfavorable ones（P＜0.001）. There was also statistical difference in PFS（7.4 mon vs. 15.2 mon）and OS（9.8 mon vs. 17.8 mon）between the B7-H3 positive group and B7-H3 negative group，respectively（P＜0.05）. Furthermore，in the AML-M2 subtype，the expression of B7-H3 on the unfavorable karyotype group（8 cases）was higher than the favorable group（29 cases，30.05% ± 23.10% vs. 10.08% ± 7.07%，P＜0.001）. There was coexpression between B7-H3 and CD34 of blast cells. The expression of B7-H3 in the CD34 positive group was higher than that in the negative group（20.90% ± 19.70% vs. 9.63% ± 7.21%，P=0.034）. Conclusion：The expression of B7-H3 in AML has relationship with the expression of the karyotype. The B7-H3 positive patients have the worse prognostic. The research of B7-H3 may be a new prognostic marker and provide insights into the leukemogenesis of acute myeloid leukemia.

参考文献

相似文献

引证文献

引用本文

吕鑫,陈仕兵,周倩,范美英,闫世彬,仇红霞.共刺激分子B7⁃H3在急性髓系白血病中的表达及生物学意义[J].南京医科大学学报（自然科学版）,2018,(1):54-58

复制

文章指标

点击次数:
下载次数:
HTML阅读次数:
引用次数:

历史

收稿日期:2016-12-12
最后修改日期:
录用日期:
在线发布日期: 2018-02-02
出版日期:

引用本文

分享

文章指标

历史

友情链接 Links