Advantageous tactics with certain probiotics for the treatment of graft-versus-host-disease after hematopoietic stem cell transplantation

Hematopoietic stem cell transplantation(HSCT)becomes a standard form of cellular therapy for patients with malignant diseases.HSCT is the first-choice of immunotherapy,although HSCT can be associated with many complications such as graft-versus-host disease(GVHD)which is a major cause of morbidity and mortality after allogeneic HSCT.It has been shown that certain gut microbiota could exert protective and/or regenerative immunomodulatory effects by the production of short-chain fatty acids(SCFAs)such as butyrate in the experimental models of GVHD after allogeneic HSCT.Loss of gut commensal bacteria which can produce SCFAs may worsen dysbiosis,increasing the risk of GVHD.Expression of G-protein coupled receptors such as GPR41 seems to be upre-gulated in the presence of commensal bacteria,which might be associated with the biology of regulatory T cells(Tregs).Treg cells are a suppressive subset of CD4 positive T lymphocytes implicated in the prevention of GVHD after allogeneic HSCT.Here,we discuss the current findings of the relationship between the modification of gut microbiota and the GVHD-related immunity,which suggested that tactics with certain probiotics for the beneficial symbiosis in gut-immune axis might lead to the elevation of safety in the allogeneic HSCT.

Unsuccessful treatment of four patients with acute graft-vs-host disease after liver transplantation

AIM: To investigate appropriate therapeutic strategies for graft-vs-host disease (GVHD) following liver transplantation. METHODS: Four patients who developed GVHD after liver transplantation in West China Hospital were included in this study. Therapeutic strategies with augmentation or withdrawal of immunosuppressants combined with supportive therapy were investigated in these patients. In addition, a literature review of patients who developed GVHD after liver transplantation was performed. RESULTS: Although a transient response to initial treatment was detected, all four patients died of complications from GVHD: one from sepsis with multiple organ failure, one from gastrointestinal bleeding, and the other two from sepsis with gastrointestinal bleeding. Few consensuses for the treatment of GVHD after liver transplantation have been reached.CONCLUSION: New and effective treatments are re-quired for GVHD after liver transplantation to improve the prognosis of patients with this diagnosis.

Age-related modifications of macrophages influenced by “inflammageing”in graft vs. host disease

Most studies focus on the adaptive immune cells in the GVHD pathogenesis,while little is known about innate immune cells in GVHD occurrence and development,especially macrophages.Meanwhile,a higher incidence of graft versus host disease(GVHD)is also found in the elderly patients.Though advances have been made in the modification of macrophages influenced by the inflamm-ageing,there is still no review on the role of macrophages in GVHD and the association between GVHD and the altered macrophages by inflamm-ageing.In this review,we focus on the potential age-related modifications of macrophage in GVHD,which contributes to the change of morbidity and mortality of GVHD.Via literature review,we found that the infiltration of macrophages is associated with GVHD and macrophages are modified in inflamm-ageing state,including the proliferation,migration,phagocytosis,antigen presentation,interaction with other immune cells,and pro-fibrosis.We suppose that altered macrophage functions in inflamm-ageing state contribute to GVHD in elderly patients.

Gut microbiome in allogeneic hematopoietic stem cell transplantation and specific changes associated with acute graft vs host disease

Allogeneic hematopoietic stem cell transplantation(aHSCT)is a standard validated therapy for patients suffering from malignant and nonmalignant hematological diseases.However,aHSCT procedures are limited by potentially life-threatening complications,and one of the most serious complications is acute graft-versus-host disease(GVHD).During the last decades,DNA sequencing technologies were used to investigate relationship between composition or function of the gut microbiome and disease states.Even if it remains unclear whether these microbiome alterations are causative or secondary to the presence of the disease,they may be useful for diagnosis,prevention and therapy in aHSCT recipients.Here,we summarized the most recent findings of the association between human gut microbiome changes and acute GVHD in patients receiving aHSCT.

Esophageal stenosis with sloughing esophagitis:A curious manifestation of graft-vs-host disease

We report a case of a 56-year-old woman with a history of allogenic bone marrow transplantation for two years,complaining with dysphagia and weight loss. Upper endoscopy revealed esophageal stenosis and extensive mucosa sloughing. Biopsies confirmed the diagnosis of graft-vs-host disease(GVHD). Balloon dilation,corticosteroids and cyclosporin resulted in marked clinical improvement. Gastrointestinal tract is involved in the majority of patients with chronic GVHD. Esophageal manifestations are rare and include vesiculobullous disease,ulceration,esophageal webs,casts or strictures. Sloughing esophagitis along with severe stenosis requiring endoscopic dilation has never been reported in this context.

Ruxolitinib add-on in corticosteroid-refractory graft-vs-host disease after allogeneic stem cell transplantation:Results from a retrospective study on 38 Chinese patients

BACKGROUND Graft-vs-host disease (GVHD) is a major cause of mortality after allogeneic hematopoietic stem cell transplantation.Some patients have steroid-refractory(SR) GVHD.AIM To evaluate the effect and safety of ruxolitinib add-on in the treatment of patients with SR acute (a) and chronic (c) GVHD.METHODS We retrospectively analyzed 38 patients administered ruxolitinib add-on to standard immunosuppressive therapy for SR-aGVHD or SR-cGVHD following allogeneic hematopoietic stem cell transplantation.Ruxolitinib was administered5-10 mg/d depending on disease severity,patient status,and the use of antifungal drugs.Overall response rate,time to best response,malignancy relapse rate,infection rate,and treatment-related adverse events were assessed.RESULTS The analysis included 10 patients with SR-aGVHD (gradeⅢ/Ⅳ,n=9) and 28patients with SR-cGVHD (moderate/severe,n=24).For the SR-aGVHD and SRcGVHD groups,respectively:Median number of previous GVHD therapies was 2(range:1-3) and 2 (1-4);median follow-up was 2.5 (1.5-4) and 5 (1.5-10) mo;median time to best response was 1 (0.5-2.5) and 3 (1-9.5) mo;and overall response rate was 100%(complete response:80%) and 82.1%(complete response:10.7%) with a response observed in all GVHD-affected organs.The malignancy relapse rates for the SR-aGVHD and SR-cGVHD groups were 10.0%and 10.7%,respectively.Reactivation rates for cytomegalovirus,Epstein-Barr virus,and varicella-zoster virus,respectively,were 30.0%,10.0%,and 0%for the SR-aGVHD group and 0%,14.3%,and 7.1%for the SR-cGVHD group.CONCLUSION Ruxolitinib add-on was effective and safe as salvage therapy for SR-GVHD.

Oral graft vs host disease:An immune system disorder in hematopoietic cell transplantation

Graft vs host disease(GVHD) is a complication of patients who are treated by hematopoietic cell transplantation.National Institutes of Health in 2005 by Working Group on Diagnosis and Staging Consensus Development Project on Criteria for Clinical Trials in Chronic GVHD(cGVHD) established 2 principal categories of oral GVHD, acute and chronic. The oral mucosa may be the first site of manifestation of the disease. Clinical diagnosis needs to be confirmed by a biopsy of oral mucosa and minor salivary glands. Microscopic results have played a major role in the diagnosis and management of acute and chronic oral GVHD. Development of second malignancies is the greatest risk of oral cGVHD patients, mostly regarding squamous cell carcinoma. The focus of oral GVHD therapy is to improve symptoms and maintain oral function. The aim of this review article is to update the information on the oral GVHD in its clinical, microscopic features and their complications.

Immunophenotypic characteristics of multipotent mesenchymal stromal cells that affect the efficacy of their use in the prevention of acute graft vs host disease

BACKGROUND Multipotent mesenchymal stromal cells(MSCs)are widely used in the clinic due to their unique properties,namely,their ability to differentiate in all mesenchymal directions and their immunomodulatory activity.Healthy donor MSCs were used to prevent the development of acute graft vs host disease(GVHD)after allogeneic bone marrow transplantation(allo-BMT).The administration of MSCs to patients was not always effective.The MSCs obtained from different donors have individual characteristics.The differences between MSC samples may affect their clinical efficacy.AIM To study the differences between effective and ineffective MSCs.METHODS MSCs derived from the bone marrow of a hematopoietic stem cells donor were injected intravenously into allo-BMT recipients for GVHD prophylaxis at the moment of blood cell reconstitution.Aliquots of 52 MSC samples that were administered to patients were examined,and the same cells were cultured in the presence of peripheral blood mononuclear cells(PBMCs)from a third-party donor or treated with the pro-inflammatory cytokines IL-1β,IFN and TNF.Flow cytometry revealed the immunophenotype of the nontreated MSCs,the MSCs cocultured with PBMCs for 4 d and the MSCs exposed to cytokines.The proportions of CD25-,CD146-,CD69-,HLA-DR-and PD-1-positive CD4+and CD8+cells and the distribution of various effector and memory cell subpopulations in the PBMCs cocultured with the MSCs were also determined.RESULTS Differences in the immunophenotypes of effective and ineffective MSCs were observed.In the effective samples,the mean fluorescence intensity(MFI)of HLAABC,HLA-DR,CD105,and CD146 was significantly higher.After MSCs were treated with IFN or cocultured with PBMCs,the HLA-ABC,HLA-DR,CD90 and CD54 MFI showed a stronger increase in the effective MSCs,which indicated an increase in the immunomodulatory activity of these cells.When PBMCs were cocultured with effective MSCs,the proportions of CD4+and CD8+central memory cells significantly decreased,and the proportion of CD8+CD146+lymphocytes increased more than in the subpopulations of lymphocytes cocultured with MSC samples that were ineffective in the prevention of GVHD;in addition,the proportion of CD8+effector memory lymphocytes decreased in the PBMCs cocultured with the effective MSC samples but increased in the PBMCs cocultured with the ineffective MSC samples.The proportion of CD4+CD146+lymphocytes increased only when cocultured with the inefficient samples.CONCLUSION For the first time,differences were observed between MSC samples that were effective for GVHD prophylaxis and those that were ineffective.Thus,it was shown that the immunomodulatory activity of MSCs depends on the individual characteristics of the MSC population.

Noninvasive tools based on immune biomarkers for the diagnosis of central nervous system graft-vs-host disease:Two case reports and a review of the literature

BACKGROUND Central nervous system graft-vs-host disease(CNS-GVHD)is a rare cause of CNS disorders after allogeneic hematopoietic stem cell transplantation.Currently,establishing a diagnosis of CNS-GVHD is challenging because the diagnostic criteria and diagnostic methods are not well defined and many confounding factors need to be ruled out.CASE SUMMARY Here,we present two patients with CNS-GVHD.Both patients with a history of acute GVHD or chronic GVHD developed neurological symptoms that could not be explained by other causes,and had abnormal cerebrospinal fluid(CSF)studies as determined by CSF and blood immune biomarker examinations,suggestive of suspected CNS-GVHD.Due to the lack of specific magnetic resonance imaging abnormalities and the rapid clinical deterioration of the patients,we did not attempt to perform a brain biopsy,but prompted the initiation of empirical immunosuppressive therapy.In view of the rapid and favorable response to local and systematic immunosuppressive treatment and the aforementioned neurologic manifestations together with CSF abnormalities and other negative findings,a final diagnosis of CNS-GVHD was made.CONCLUSION CSF and blood immune biomarker examinations facilitated the diagnosis of CNSGVHD,which are particularly suitable for patients who are critically ill and require urgent treatment and for those who are unsuitable for invasive diagnostic procedures.

Immune Regulatory Cell Biology and Clinical Applications to Prevent or Treat Acute Graft-Versus-Host Disease

The most common approaches to prevent and treat graft-versus-host disease (GVHD) are intended to deplete or suppress the T cells capable of mediating or supporting alloresponses;however, this renders the recipients functionally T cell deficient and hence highly susceptible to infections and tumor recurrence. Depletion is often accomplished through the use of broadly reactive antibodies, while functional impairment is typically achieved by pharmacological agents that require long-term administration (usually six months or more), have significant side effects, and may not result in tolerance (i.e., nonresponsiveness) of donor T cells to conditioning regimen-resistant host alloantigen-bearing cells. As our knowledge of immune system homeostasis has increased, cell populations with immune regulatory function have been identified and characterized. Although such cell populations are typically present in low frequencies, methods to isolate and expand these cells have permitted their supplementation to the donor graft or infusion late post-transplant in order to stifle GVHD. This review discusses the biology and preclinical proof of concept of GVHD models, along with GVHD outcomes that focus exclusively on immune regulatory cell therapies that have progressed to clinical testing.

allo-HSCT后淋巴细胞亚群重建与GVHD及感染的相关性

目的探讨血液病病人异基因造血干细胞移植(allo-HSCT)后外周血淋巴细胞各亚群的重建规律,以及淋巴细胞各亚群变化与移植后移植物抗宿主病(GVHD)及感染的关系。方法采用流式细胞术,检测32例allo-HSCT病人清髓处理前3 d和移植后14、30、90、180、365、730 d时的淋巴细胞亚群分布情况,并分析病人GVHD以及感染与淋巴细胞各亚群变化的关系。结果与移植前比较,血液病病人移植后总淋巴细胞、CD3^(+)T细胞、CD4^(+)T细胞、CD8^(+)T细胞、CD16^(+)CD56^(+)NK细胞、CD19^(+)B细胞重建的速度不同,其中NK细胞恢复最快,不到30 d就恢复至移植前水平;其次为CD8^(+)T细胞,约30 d恢复至移植前水平;CD3^(+)T细胞在移植后60 d基本可以达到移植前水平;而B细胞以及CD4^(+)T细胞恢复较慢,B细胞约360 d恢复至移植前水平,CD4^(+)T细胞在移植后730 d仍未恢复到移植前水平。移植后第90天,发生急性移植物抗宿主病(aGVHD)病人5例,其CD3^(+)T细胞(t’=3.334,P<0.05)、CD4^(+)T细胞(t=3.836,P<0.05)和CD16^(+)CD56^(+)NK细胞(t=3.300,P<0.05)绝对计数均低于非急性移植物抗宿主病(non-aGVHD)组,差异有统计学意义。移植后第365天,发生慢性移植物抗宿主病(cGVHD)病人17例,其CD4^(+)T细胞计数低于非慢性移植物抗宿主病(non-cGVHD)组,差异有统计学意义(t=2.918,P<0.05)。与无感染组(n=5)比较,移植后第180天病毒感染组(n=6)淋巴细胞(t=2.441,P<0.05)、CD4^(+)T细胞(t=3.513,P<0.05)、NK细胞(t=3.728,P<0.05)、B细胞(t=2.937,P<0.05)降低;细菌感染组(n=8)淋巴细胞(t=2.535,P<0.05)、CD4^(+)T细胞(t’=6.726,P<0.05)降低,CD8^(+)T细胞升高(t’=-2.945,P<0.05);真菌感染组(n=4)CD4^(+)T细胞降低(t=2.579,P<0.05),CD8^(+)T细胞升高(t=2.423,P<0.05);混合感染组(n=9)淋巴细胞(t=2.195,P<0.05)、CD3^(+)T细胞(t=2.649,P<0.05)、CD4^(+)T细胞(t=3.728,P<0.05)、CD8^(+)T细胞(t=2.579,P<0.05)、B细胞(t=3.045,P<0.05)和NK细胞(t=2.207,P<0.05)绝对计数均降低。结论allo-HSCT后淋巴细胞各亚群的重建以及变化与病人预后相关,应该连续监测病人移植前后外周血淋巴细胞亚群的变化情况。

0.05%环孢素与0.1%他克莫司滴眼液治疗慢性oGVHD后患者眼表干眼相关指标及泪液炎症因子比较

目的比较0.05%环孢素与0.1%他克莫司滴眼液治疗慢性眼部移植物抗宿主病(oGVHD)后患者眼表干眼相关指标及泪液炎症因子的改变。方法采用随机对照研究方法,纳入2020年4月至2021年4月于北京大学第三医院眼科确诊为慢性oGVHD的患者60例60眼,采用随机数字表法将患者分为他克莫司组30例30眼和环孢素组30例30眼。他克莫司组主要采用0.1%他克莫司滴眼液点眼,2次/日;环孢素组采用0.05%环孢素滴眼液点眼,4次/日。此外,2个组患眼均采用0.1%氟米龙滴眼液2次/日、小牛血去蛋白提取物眼用凝胶3次/日、0.1%玻璃酸钠滴眼液8次/日点眼,进行抗炎和润滑治疗。用药后1个月随访并依据排除标准筛选患者,最终将他克莫司组21例21眼和环孢素组12例12眼纳入后续研究。分别于治疗前、治疗后1个月对患眼进行检查,主要评价指标包括眼表疾病指数(OSDI)问卷评分、角膜荧光素钠染色评分和泪膜破裂时间(BUT)。采用Luminex芯片法检测患眼治疗前后泪液中白细胞介素(IL)-6、IL-8、IL-17、表皮生长因子(EGF)和肿瘤坏死因子-α(TNF-α)的质量浓度并进行组间比较。结果他克莫司组和环孢素组治疗前后OSDI差值分别为0.4(-5.6,21.5)和27.2(4.6,45.0),环孢素组OSDI改善程度明显优于他克莫司组,差异有统计学意义(Z=-2.547,P=0.009)。他克莫司组和环孢素组治疗前后角膜荧光素钠染色评分差值分别为5.0(2.5,10.0)分和3.5(-0.5,13.8)分,BUT差值分别为0.0(-3.0,0.0)s和-1.5(-3.0,0.0)s,组间比较差异均无统计学意义(Z=-0.526、-0.804,均P>0.05)。他克莫司组与环孢素组治疗前后IL-6、IL-8、IL-17、EGF和TNF-α表达量差值比较,差异均无统计学意义(Z=-0.487、-0.112、-0.412、-1.085、-1.198,均P>0.05)。结论2种药物治疗慢性oGVHD后,患者泪液中各因子含量的改变程度均未见显著差异。慢性oGVHD患者应用0.05%环孢素滴眼液治疗可能比0.1%他克莫司滴眼液有更好的舒适度。

Gene and protein expression of proteinase-activated receptor-1, 2 in a murine model of acute graft vs host disease

Proteinase-activated receptors(PARs)are a novel subclass of seven transmembrane-spanning,G protein-coupled receptors.PAR-1 and PAR-2 are widely expressed in a variety of cells and are found to be involved in many physiological and pathological processes includ-ing inflammation and immune response.However,little is known about the function of PAR-1,2 in acute graft vs host disease(GVHD).In the present study,wefirst detected the expression of PAR-1,2 protein and mRNA in a murine model of acute GVHD using the methods of immunohis-tochemistry,Western blot and quantitative real-time polymerase chain reaction(PCR).Syngeneic hematopoie-tic stem cell transplantation(HSCT)mice served as controls.The relative gene expression level of PAR-1 was significantly increased in the skin,liver,small intestine of allogeneic HSCT mice(in skin:0.039�0.013 vs 0.008�0.002 of controls,P=0.009;in liver:0.165�0.006 vs 0.017�0.006 of controls,P=0.004;in small intestine:0.215�0.009 vs 0.016�0.002 of con-trols,P=0.003),but not in the stomach,lung and kidney of allogeneic HSCT mice(P>0.05).PAR-2 mRNA expression in the liver and small intestine of allogeneic HSCT mice(in liver:0.010�0.002 vs 0.003�0.001 of controls,P=0.008;in small intestine:0.006�0.001 vs 0.003�0.001 of controls,P=0.024)was increased significantly,but PAR-2 mRNA expression in the other organs(P>0.05)was not found to be significantly elevated.PAR-1,2 protein expression was in accordance with the mRNA expression,as shown by Western blot.Using immunohistochemistry the present study demon-strated that there was strong PAR-1,2 immunoreactivity in the epithelial cell and vascular endothelial cell of target organs of acute GVHD.Ourfindings of markedly increased expression of PAR-1,2 in target organs of acute GVHD suggest that PAR-1 and PAR-2 may play an important role in the pathogenesis of acute GVHD.

EL9611红白血病小鼠急性GVHD动物模型的建立

目的:建立EL9611红白血病小鼠急性移植物抗宿主病(GVHD)的动物模型。方法:同种异基因骨髓移植(allo-BMT)以C57BL/6(H-2b)鼠为供鼠,BALB/c(H-2d)为受鼠。设白血病组(n=10)、照射对照组(白血病鼠照射后不进行allo-BMT,n=4)、GVHD组(白血病鼠照射+allo-BMT,n=10)及正常对照组(n=4)。白血病组采用每只BALB/c鼠尾静脉输注2×106个EL9611红白血病细胞建立红白血病动物模型;GVHD组于接种白血病细胞7 d后行总剂量为8.0 Gy的1次性[60Co]γ射线全身照射(TBI),照射后5 h内每只小鼠尾静脉输注C57BL/6鼠骨髓细胞2×106个+脾细胞1×107个,建立EL9611红白血病小鼠的急性GVHD动物模型。观察小鼠体位、皮毛、大便等临床表现,病理检查肝脾、皮肤、小肠、外周血和骨髓,计算生存率。结果:白血病组生存时间(14.5±2.1)d[从照射当天(第0 d)算起为(7.5±0.7)d],生存时间与GVHD组相比P<0.01,死亡率100%,无自发缓解,死亡时肝脾肿大(肝重2.40 g±0.48 g,脾重0.84 g±0.20 g,与正常对照组比P<0.01),外周血WBC升高[死亡前(3.33±0.27)×1010/L,与正常对照组比P<0.05],病理检查示组织正常结构破坏,白血病细胞浸润。照射对照组生存时间为(9.0±0.7)d,生存时间与GVHD组和正常对照组相比差异显著(P<0.01),死亡率100%,病理检查显示造血衰竭。GVHD组生存时间为(32.0±3.2)d,生存时间与其它各组相比P<0.01,死亡率100%,allo-BMT后第10-13 d出现症状,临床表现和病理检查符合Ⅰ到Ⅱ度GVHD的改变。结论:采用EL9611红白血病细胞(2×106/鼠)静脉输注的方式可成功建立EL9611红白血病动物模型;接种EL9611红白血病细胞第7d行TBI+allo-BMT可成功建立EL9611红白血病小鼠的急性GVHD动物模型。

CT增强扫描鉴别异基因骨髓移植术后腹部GVHD和机遇性感染（英文）

目的:比较骨髓移植术后腹腔移植物抗宿主病(GVHD)和机遇性感染的CT表现以确定有助于鉴别诊断的CT特点。方法:纳入25例腹腔GVHD和15例腹腔机遇性感染患者,机遇性感染包括巨细胞病毒性感染(n=4)、真菌性感染(n=6)及细菌性感染(n=5)。对所有病人进行CT扫描。CT征象包括肠壁增厚、异常黏膜增强、肠管扩张、大量积液、胆管扩张、腹水以及邻近肠系膜条状征。分析病变的位置和范围。对两组病人的CT征象进行对照分析。结果:在胃肠道不连续性多发分布多见于GVHD;而连续性分布多见于机遇性感染(P<0.05)。胆管扩张是GVHD最常见的肠道外病变,然而非常少见于机遇性感染(P<0.05)。皮肤斑丘疹见于60%的GVHD,但是不见于机遇性感染(P<0.05)。对没有皮肤病变的病人,肠管病变的不连续分布和胆管扩张更多见于GVHD。结论:GVHD和机遇性感染的CT征象有较大重叠,尽管如此,一些临床和CT征象,例如皮肤斑丘疹、胆管扩张和肠管病变的不连续多发分布有利于诊断GVHD。

不完全相合造血干细胞移植中GVHD的预测研究:模拟HLA抗原结构的比较与应用

采用通用的微量淋巴细胞毒实验和序列测定方法对拟进行造血干细胞移植的患者及供体进行HLA分型 ;用计算机分子模拟手段 ,从HLA分子三维结构方面探讨预测移植物抗宿主病 (GVHD)发生程度 ,以预测移植后GVHD的发生情况。结果发现 ,8例供受体中 ,3例为半匹配移植 ,其中 2例发生了Ⅳ度GVHD ,1例发生了Ⅱ度GVHD ;3例为两个抗原不相合移植 ,其中 1例发生了Ⅱ度GVHD ,2例发生了Ⅱ度GVHD ;2例患者为一个抗原不相合移植 ,分别发生了Ⅰ度、Ⅱ度GVHD ;GVHD的发生程度与HLA不相合抗原RMSD差异的大小呈正相关。提示异基因造血干细胞移植时 ,GVHD发生程度与HLA分子三维结构的差异有密切关系 。

脂肪源间充质干细胞治疗aGVHD分子机制的初步研究

目的初步探讨成人脂肪源间充质干细胞(adultadiposetissue-derivedmesenchymalstemcells,AMSC)治疗急性移植物抗宿主病(acutegraft-versus-hostdisease,aGVHD)的分子机制。方法3例行异基因造血干细胞移植术后发生aGVHD患者,以每公斤体质量2×106个细胞剂量静脉输注AMSC;应用RT-PCR扩增患者AMSC使用前后外周血单个核细胞的TCRVβ24个亚家族的CDR3,了解患者TCRVβT细胞的分布情况;应用尼龙毛柱分离外周血T淋巴细胞再经CD8磁珠分选出CD8+T淋巴细胞,应用流式细胞术检测发生aGVHD患者使用AMSC前后外周血CD8+T细胞亚群的变化。结果患者发生aGVHD时,有TCRVβ3及其他亚家族基因表达,输注AMSC后,GVHD得以有效控制,Vβ不表达;当患者GVHD复发时,Vβ3基因又表达,治疗后不表达;与输注AMSC前相比,输注AMSC后,CD8+T细胞中的CD8+CD28-亚群显著上调(P<0.05),同时,患者的aGVHD得以有效控制。结论AMSC治疗aGVHD的分子机制可能与其抑制TCRVβ亚家族基因表达有关,TCRVβ3可能是AMSC作用的靶基因;同时,AMSC治疗aGVHD的作用机制可能与其上调CD8+CD28-T细胞亚群有关,CD8+T细胞可能是AMSC作用的靶细胞。

实时定量PCR检测GVHD患者TCR V_γ亚家族基因表达水平

目的了解异基因造血干细胞移植后移植物抗宿主病(GVHD)疾病状态下T细胞受体(TCR) Vγ亚家族T细胞水平的变化情况。方法采用实时荧光定量聚合酶链反应对18例GVHD患者外周血单个核细胞TCR VγI～III亚家族基因表达水平进行相对定量检测;12例健康成人外周血样本作为对照。结果GVHD患者外周血中TCR VγII的表达量显著低于正常对照;GVHD患者TCR VγI～III亚家族的表达模式也发生了改变,TCR VγII的表达量比TCR VγI或TCR VγIII的表达量低。结论TCR VγII亚家族的表达低下可能与GVHD的发病相关。

活化半相合混合骨髓移植GVHD反应的动物实验研究

目的:观察活化半相合混合骨髓移植的GVHD反应。方法:以急性放射病615小鼠模型为受鼠,615×C57BL/6杂交F1代小鼠为半相合供鼠。半相合鼠骨髓和脾细胞中混合一定比例的同基因脾细胞,经白细胞介素-2体外活化后,进行活化半相合混合骨髓移植。观察移植后小鼠死亡率、白细胞系造血重建、脾结节、体内混合淋巴细胞培养、嵌合体及病理学改变,比较不同移植方式的GVHD反应。结果:活化半相合骨髓移植组与未活化半相合骨髓移植组具有明显的GVHD反应。供受鼠3:1活化半相合混合骨髓移植不能明显降低GVHD反应,供受鼠脾细胞比例1:1和2:1移植组可以明显减轻GVHD反应。表现为外周血自细胞及骨髓造血恢复快,体内混合淋巴细胞反应降低及嵌合体百分率升高。结论:活化半相合混合骨髓移植方式可以降低GVHD反应,并与同基因和异基因脾细胞比例有关。

胃肠型GVHD患者不同营养方案的临床疗效

目的比较不同营养支持方案对胃肠道移植物抗宿主病(GVHD)患者营养状况改善的作用,并对不同营养方案进行评价,观察不同营养方案对胃肠道GVHD辅助治疗的疗效。方法对35例胃肠道GVHD患者随机分为完全肠外营养组(TPN)和经口饮食组(OD),分别于治疗后的0、14、28 d评价患者的营养状况和GVHD临床疗效。结果 35例胃肠道GVHD患者在治疗后14、28 d均为负氮平衡。患者的GVHD临床症状缓解率显示,TPN组大于OD组,P<0.05。结论胃肠道GVHD患者属于营养不良状况,并且随着疾病时间的延长,营养不良状况加重,加重的程度TPN组最慢。TPN有助于抗胃肠道GVHD治疗。