间充质干细胞移植后免疫重建和抗巨细胞病毒的免疫作用

背景:异基因造血干细胞移植是治愈白血病等恶性血液病、重症再生障碍性贫血和遗传性血液病的最有效方法,但移植后早期常因免疫重建延迟,显著增加巨细胞病毒感染/再激活的风险。只有促进早期免疫重建,才能激发机体产生巨细胞病毒特异性免疫应答,真正有效的长期控制病毒复制。目的:总结间充质干细胞移植后免疫重建和抗巨细胞病毒免疫作用的研究进展,并分析目前面临的问题及其未来发展方向。

抗人巨细胞病毒免疫球蛋白G在脑胶质瘤的表达及与预后的相关性

目的:探讨抗人巨细胞病毒免疫球蛋白G(HCMV IgG)水平在脑胶质瘤的表达及与预后的相关性。方法:选择2013年1月至2017年8月在我院就诊并接受手术切除的脑胶质瘤患者作为研究对象,入组后测定患者抗HCMV IgG水平,观察抗HCMV IgG表达及水平与脑胶质瘤患者特征与预后的相关性。结果:患者抗HCMV IgG阳性表达率为76.17%。抗HCMV IgG与年龄、性别、肿瘤部位、肿瘤大小、病程、KPS评分等均无相关性(P>0.05),与肿瘤分级存在正相关(P<0.05)。肿瘤分级、手术方式、替莫唑胺疗程和抗HCMV IgG表达是影响患者1年死亡率的独立预后因素(P均<0.05)。对IgG阳性患者进一步分析显示,抗HCMV IgG<10 U/ml患者生存期低于10~29 U/ml和≥30 U/ml患者(P<0.05),抗HCMV IgG≥30 U/ml患者生存期高于10~29 U/ml患者但差异无统计学意义(P>0.05)。结论:抗HCMV IgG表达与胶质瘤恶性程度呈正相关,与生存期呈负相关,抗HCMV IgG低表达患者具有更差的预后,应引起临床关注。

更昔洛韦对不孕不育患者巨细胞病毒感染的疗效评价

目的:评价更昔洛韦对不孕不育女性患者巨细胞病毒(CMV)感染的临床疗效。方法:选取2013年12月—2015年12月收治的不孕不育CMV感染患者60例作为研究对象,以患者入院时间先后将其分为A组和B组,每组30例;A组患者均给予更昔洛韦注射液治疗,B组患者均给予抗巨细胞病毒的免疫球蛋白制剂治疗,比较两组患者治疗后的临床疗效以及不良反应的发生率。结果:治疗后,A组患者的巨细胞病毒(CMV-DNA)和CMV抗体(CMV-IgM)转阴率以及受孕率优于B组患者(P<0.05),不良反应的发生率与B组患者比较其差异无统计学意义(P>0.05)。结论:对不孕不育CMV感染妇女,采用更昔洛韦注射给药治疗的疗效和安全性均较好。

Diagnostic value of antigenemia assay for cytomegalovirus gastrointestinal disease in immunocompromised patients

AIM:To investigate the utility of the cytomegalovirus(CMV)antigenemia assay for the diagnosis of CMV gastrointestinal disease(GID). METHODS:One hundred and thirty immunocompromised patients were enrolled in this study.Patients with a history of anti-CMV treatment and who had not undergone examination using the antigenemia assay were excluded.CMV-GID was defined as the detection of large cells with intranuclear inclusions alone or associated with granular cytoplasmic inclusions by biopsy.Biopsy sections were stained with hematoxylin and eosin and immunohistochemically stained with anti-CMV.We evaluated the association between CMV-GID and patient characteristics(symptoms,underlying disease,medication,leukocyte counts,and antigenemia assay).All patients were checked with an human immunodeficiency virus(HIV)antibody test before endoscopic examination.White blood cell(WBC)counts were obtained from medical records within 1 wk of endoscopy.Leukopenia was defined as a total WBC count<5000 cells/mm 3 . For HIV patients,we also checked CD4+counts from medical records. RESULTS:A total of 99 patients were retrospectively selected for analysis.Of the immunocompromised patients,19 had malignant disease,18 had autoimmune disease,19 had disorders of biochemical homeostasis, three had undergone transplantation,and 45 had HIV infection.A total of 50 patients had received immunosuppressive therapy.No patients had inflammatory bowel disease.Fifty-five patients were diagnosed as having CMV-GID.Univariate analysis indicated an association between HIV infection,leukopenia,and positive antigenemia and CMV-GID(P<0.05).Multivariate analysis using logistic regression revealed that HIV infection and positive antigenemia were the only independent factors related to CMV-GID(P<0.01).The sensitivity,specificity,positive predictive value,and negative predictive value of antigenemia for CMV-GID were 65.4%,93.6%, 91.9%,and 71.0%,respectively.In a subgroup analy-sis,patients with leukopenia displayed low sensitivity and high specificity.Minimal differences in accuracy were seen among patients with or without leukopenia. HIV-infected patients displayed low sensitivity and high specificity.Accuracy barely differed between HIV-positive and-negative patients.In HIV-infected patients, CD4 count<50 cells/μL resulted in low sensitivity and high specificity.Differences in accuracy among patients were minor,regardless of CD4 count.In patients who had undergone both quantitative real-time polymerase chain reaction(PCR)and antigenemia assay,real-time PCR was slightly more accurate in terms of sensitivity than the antigenemia assay;however,this difference was not statistically significant(P=0.312). CONCLUSION:If the antigenemia test is positive,endoscopic lesions are acceptable for the diagnosis of CMVGID without biopsy.The accuracy is not affected by HIV infection and leukopenia.Either PCR or the antigenemia assay are valid.