A New Immunosuppressive Therapy for Very Severe Aplastic Anemia in Children with Autoantibodies

Objective At present,a number of very severe aplastic anemia(VSAA)patients cannot receive hematopoietic stem cell transplantation(HSCT)or standard immunosuppressive therapy(IST)due to the high cost of therapy,shortage of sibling donors,and lack of resources to support the HSCT.In addition,some VSAA patients with autoantibodies have no life-threatening infections or bleeding at the time of initial diagnosis.Considering the disease condition,economics and other factors,the present study designed a new and relatively mild treatment strategy:cyclosporine A plus pulsed high-dose prednisone(CsA+HDP).Methods The present study retrospectively analyzed 11 VSAA patients,who were treated with CsA+HDP in our hospital from August 2017 to August 2019.Results The median follow-up time for these patients was 24.9 months.The overall response rate was 54.5%(6/11)at six months after the initiation of IST and 81.8%(9/11)at deadline.Five patients achieved complete remission and four patients met the criteria for partial response at the last follow-up.The median time to response for responders was 110 days.Three patients underwent HSCT due to the poor effect of CsA+HDP or to find a suitable transplant donor.Recurrence and clonal evolution were not found in any of these patients.The estimated 3-year overall survival rate and 3-year failure-free survival rate were 100.0%and 72.7%,respectively.In addition,the results revealed that the cyclosporine-prednisone-associated toxicity was mild and well-tolerated by most patients.Conclusion The novel CsA+HDP regimen has good therapeutic effect and safety for VSAA patients with autoantibodies,who have no serious life-threatening infections or bleeding at the time of initial diagnosis.

Yin and Yang of mesenchymal stem cells and aplastic anemia

Acquired aplastic anemia(AA) is a bone marrow failure syndrome characterized by peripheral cytopenias and bone marrow hypoplasia. It is ultimately fatal without treatment, most commonly from infection or hemorrhage. Current treatments focus on suppressing immune-mediated destruction of bone marrow stem cells or replacing hematopoietic stem cells(HSCs) by transplantation. Our incomplete understanding of the pathogenesis of AA has limited development of targeted treatment options. Mesenchymal stem cells(MSCs) play a vital role in HSC proliferation; they also modulate immune responses and maintain an environment supportive of hematopoiesis. Some of the observed clinical manifestations of AA can be explained by mesenchymal dysfunction. MSC infusions have been shown to be safe and may offer new approaches for the treatment of this disorder. Indeed, infusions of MSCs may help suppress auto-reactive, T-cell mediated HSC destruction and help restore an environment that supports hematopoiesis. Small pilot studies using MSCs as monotherapy or as adjuncts to HSC transplantation have been attempted as treatments for AA. Here we review the current understanding of the pathogenesis of AA and the function of MSCs, and suggest that MSCs should be a target for further research and clinical trials in this disorder.

Early Detection of Myelodysplastic Syndrome/Leukemia-associated Mutations Using NGS Is Critical in Treating Aplastic Anemia

Distinguishing between aplastic anemia(AA)and hypoblastic myelodysplastic syndrome(hMDS)with a low percentage of bone marrow(BM)blasts(<5%)can be difficult due to the overlap in clonality and a spectrum of genetic alternations between the two subtypes of diseases.However,due to recent advances in DNA sequencing technology,both spectnim and frequency of mutations can be accurately determined and monitored by next-generation sequencing(NGS)at initial diagnosis and during immunosuppressive therapy(1ST)in patients with AA or hMDS.This improvement in acquiring a patient's genetic status and clonal evolution can provide more proper,precise,and on-time information to guide disease management,which is especially helpful in the absence of traditional morphologic/cytogenetic evidence.

Epstein–Barr-virus-associated hepatitis with aplastic anemia: A case report

BACKGROUND Hepatitis-associated aplastic anemia(HAAA) is a rare condition. Patients with HAAA usually present with acute hepatitis, jaundice and significantly increased transaminase. After 1–2 mo, hepatitis gradually improves, but progressive hemocytopenia, bone marrow hematopoietic failure, and severe or extremely severe aplastic anemia are manifest. Most cases of HAAA are fulminant and usually lethal if left untreated. The literature on Epstein–Barr virus(EBV)-associated HAAA is sparse.CASE SUMMARY We report a 30-year-old man who was admitted to our hospital because of pale yellow urine and skin with a simultaneous decrease in peripheral blood ternary cells. We made a diagnosis of EBV-associated HAAA. The treatment strategy for this patient included eltrombopag, an immunosuppressive regimen of rabbit antihuman thymocyte immunoglobulin, cyclosporine, and supportive care. The patient was discharged in normal physical condition after five months. A hemogram performed on follow-up revealed that he had achieved a complete response.CONCLUSION Eltrombopag plus anti-thymocyte globubin and cyclosporine may be a therapeutic option for EBV-associated HAAA.Larger studies are warranted to confirm.

TREATMENT OF APLASTIC ANEMIA: ALLOGENEIC BONE MARROW TRANSPLANTATION VERSUS IMMUNOMODULATION THERAPY WITH ANTILYMPHOCYTE GLOBULIN

There are two arms in the management of aplastic anemia,one allogeneic bone marrow transplantation(BMT) and the other immunomodulation therapy with antilymphocyte globulin(ALG).

An investigation of long-term outcome of rabbit anti-thymocyte globulin and cyclosporine therapy for pediatric severe aplastic anemia

Children with severe aplastic anemia(SAA)face heterogeneous prognoses after immunosuppressive therapy(IST).There are few models that can predict the long-term outcomes of IST for these patients.The objective of this paper is to develop a more effective prediction model for SAA prognosis based on clinical electronic medical records from 203 children with newly diagnosed SAA.In the early stage,a novel model for long-term outcomes of SAA patients with IST was developed using machine-learning techniques.Among the indicators related to long-term efficacy,white blood cell count,lymphocyte count,absolute reticulocyte count,lymphocyte ratio in bone-marrow smears,C-reactive protein,and the level of IL-6,IL-8 and vitamin B12 in the early stage are strongly correlated with long-term efficacy(P<.05).Taken together,we analyzed the long-term outcomes of rabbit antithymocyte globulin and cyclosporine therapy for children with SAA through machine-learning techniques,which may shorten the observation period of therapeutic effects and reduce treatment costs and time.

Advances and perspectives on cellular therapy in acquired bone marrow failure diseases

Acquired bone marrow failure diseases(ABMFD) are a class of hematopoietic stem cell diseases with a commonality of non-inherited disruption of hematopoiesis that results in pancytopenia. ABMFDs also are a group of heterogeneous diseases with different etiologies and treatment options. The three most common ABMFDs are aplastic anemia, myelodysplastic syndrome, and paroxysmal nocturnal hemoglobinuria. Stem cell transplantation is the only treatment that can cure these diseases. However, due to high therapy-related mortality, stem cell transplantation has rarely been used as a first line treatment in treating ABMFD. With the advance of personalized medicine and precision medicine, various novel cellular therapy strategies are in trial to increase the efficiency and efficacy of ABMFD treatment. This article aims to review current available stem cell transplantation protocols and promising cellular therapy research in treating ABMFD.

Effect on Life Span and Membrane Protein in Red Blood Cells by Integrated Medicine Therapy on Chronic Aplastic Anemia

Objective: To explore the mechanism ofintegrated traditional Chinese and Westernmedicine (TCM--WM ) therapy on chronicaplastic anemia (CAA). Methods: The RBClife span of 30 normal human subjects and 30patients with CAA were measured by sir labelled technique before and after TCM--WMtherapy. The morphology and distribution ofRBC membrane protein granules were observed by freeze fracture etching and transmission electron microscope. Results: The halflife of erythrocytes (RBC TI/2)was shortenedin CAA cases and there was a significant difference compared to healthy control (P <0. 01). After therapy, the RBC life span prolonged and approached the normal level. Before treatment, there existed abnormal in morphology, decrease in amount and uneven indistribution of protein granules in protoplasmicface (PF) and extracellular face (EF) of RBCmembrane. After treatment, the protein granules of RBC membrane was improved and approached to control. Conclusions: The morphology, amount, quality and distribution ofRBC membrane protein granule were closelyrelated to its life span. The therapeutic effectof TCM--WM was better than that of WMalone and it had a function both in stabilizingmembrane protein and extending the RBC lifespan.

基于德尔菲法构建再生障碍性贫血患者的健康教育方案

目的 基于德尔菲法构建再生障碍性贫血(AA)患者的健康教育方案,以期为AA患者提供科学的、合理的健康教育指导。方法 以知信行为理论基础,通过文献回顾、半结构式访谈法拟定健康教育方案的初稿,选取15名专家运用德尔菲法开展2轮咨询,基于专家建议对初稿的条目及维度进行修改,最终构建基于知信行理论的AA患者健康教育方案。结果 2轮专家函询问卷回收率均为100%;2轮专家函询中的专家权威程度(Cr)分别为0.893、0.885。第1轮函询中一级条目、二级条目、三级条目专家肯德尔协调系数分别为0.572、0.546、0.512(P<0.05),重要性赋值均数均大于2.97分,变异系数为0.05~0.23,满分率为19.95%~93.42%;第2轮函询中一级条目、二级条目、三级条目专家肯德尔协调系数分别为0.681、0.679、0.548(P<0.05),重要性赋值均数均大于4.08分,变异系数为0.00~0.17,满分率为25.00%~100.00%。最终形成AA患者的健康教育方案[包括3个一级指标(健康知识、健康信念、健康行为)、16个二级指标、55个三级指标]。结论 该研究构建的健康教育方案可信程度较高,指标体系权威性好,权重合理。

重型再生障碍性贫血治疗的研究进展

重型再生障碍性贫血(SAA)是一种急性且致命性的骨髓衰竭症,其发展速度快且病死率较高,预期结果较差。使用抗淋巴/胸腺细胞球蛋白联合环孢素作为标准疗法来控制再生障碍性贫血(AA)已经成为普遍做法,近年来雄激素、艾曲泊帕等药物的应用使得SAA患者的生存率显著升高。对于那些无法耐受或者再次出现病情恶化的病人来说,可以选择做同种异体造血干细胞移植(HSCT)以获得更好的疗效。HSCT前预处理方法的改进及移植后各种药物的应用,使得移植的成功率升高,移植物抗宿主病的发生率降低,异基因造血干细胞移植已成为临床研究的热门。本研究总结SAA近年来的移植和非移植治疗,分析其疗效及相关优缺点。

补肾活血法联合环孢素及雄激素治疗再生障碍性贫血的有效性及安全性的Meta分析

【目的】系统性评价补肾活血法联合环孢素及雄激素方案治疗再生障碍性贫血(aplastic anemia,AA)的临床有效性和安全性。【方法】检索国内外主要数据库中采用补肾活血法联合环孢素及雄激素(试验组)对比环孢素及雄激素(对照组)治疗AA的随机对照试验(randomized controlled trials,RCTs),筛选符合纳入标准的高质量RCTs,采用RevMan 5.3软件进行Meta分析。【结果】共纳入6项研究,涉及365例患者。Meta分析结果显示,试验组治疗AA总有效率显著优于对照组[OR=4.43,95%CI(2.50,7.84);P<0.00001],试验组在改善外周血象指标如血红蛋白(HGB)水平[MD=14.85,95%CI(10.66,19.05);P<0.00001]、白细胞(WBC)水平[MD=0.61,95%CI(0.21,1.01);P=0.003]、血小板(PLT)水平[MD=16.51,95%CI(9.28,23.75);P<0.00001]等方面优于对照组,且未增加多毛症发生率[OR=0.24,95%CI(0.10,0.61);P=0.003]、痤疮发生率[OR=0.30,95%CI(0.13,0.66);P=0.003]、肝功能异常发生率[OR=0.28,95%CI(0.09,0.83);P=0.02]等不良反应。【结论】补肾活血法联合环孢素及雄激素治疗AA在提高临床疗效、改善外周血象方面均优于单纯使用环孢素及雄激素治疗,同时在减轻不良反应方面有一定优势。

补肾生血汤联合常规西药治疗再生障碍性贫血患者的效果

目的:观察补肾生血汤联合常规西药治疗再生障碍性贫血(AA)患者的效果。方法:选取2021年7月至2023年6月该院收治的84例AA患者进行前瞻性研究,按随机数字表法将其分为对照组与观察组各42例。对照组予以常规西药治疗,观察组在对照组基础上联合补肾生血汤治疗。比较两组临床疗效,治疗前后外周血象指标[血红蛋白(Hb)、血小板计数(PLT)、白细胞计数(WBC)、中性粒细胞计数(ANC)]水平、中医证候积分、白细胞介素(IL;IL-6、IL-10)水平,以及不良反应发生率。结果:观察组治疗总有效率为88.10%(37/42),高于对照组的69.05%(29/42),差异有统计学意义(P<0.05);治疗后,两组Hb、PLT、WBC、ANC水平均高于治疗前,且观察组高于对照组,差异有统计学意义(P<0.05);两组中医证候积分均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05);两组IL-6、IL-10水平均低于治疗前,且观察组低于对照组,差异有统计学意义(P<0.05);治疗期间,两组均未发生明显不良反应。结论:补肾生血汤联合常规西药治疗AA患者可提高治疗总有效率,改善外周血象指标水平,降低中医证候积分和IL水平的效果优于单纯常规西药治疗。

当归补血汤治疗慢性贫血临床观察

目的分析当归补血汤对治疗性贫血患者的临床疗效。方法选择侯马市人民医院2022年5月—2023年5月收治的80例慢性贫血患者,分为研究组和对照组,各40例。2组均接受红细胞输血治疗,研究组提供当归补血汤干预,对照组则提供常规干预。对比2组治疗后贫血改善、凝血状况、中医证候积分、功能状态和治疗安全性。结果研究组贫血状态改善、功能状态评分、治疗安全性及中医证候积分均优于对照组(P<0.05);2组凝血功能对比,差异无统计学意义(P>0.05)。结论当归补血汤应用于慢性贫血患者治疗中,可尽早改善贫血,提升免疫力,提高治疗安全性。

Aplastic anemia associated with dyskeratosis congenita treated with antilymphocyte globulin and cyclosporine: a case report

Dyskeratosis congenita (DC) is a severe inherited disease characterized by a triad of clinical manifestations including abnormal skin pigmentation, nail dystrophy, and mucosal leukoplakia. 1 Bone marrow failure is the principal cause of early mortality, together with an increased predisposition to malignancy and fatal pulmonary complications. According to the dyskeratosis congenita registry, a peripheral blood cytopenia of one or more lineages is reported in 93% of patients, with 51% developing pancytopenia before the age of 10 years. 2 In patients with DC, bone marrow failure or bone marrow failure treatment-associated complications account for 67% of total mortality. 3 Therefore, management of bone marrow failure syndrome is crucial in patients with DC.

慢性再生障碍性贫血CD8^+T细胞CD28表达与中医辨证分型关系的探讨

目的探讨慢性再生障碍性贫血 (chronicaplasticanemia ,CAA)患者外周血CD8+T细胞CD2 8分子的表达与中医辨证分型的关系。方法采用流式细胞仪技术 ,测定门诊和住院CAA患者 4 5例、健康对照人群 2 4名的外周血CD8+T细胞CD2 8分子的表达水平 ,从免疫学角度讨论其与中医分型关系。结果(1)CAA患者的CD8、CD2 8、CD8+CD2 8+表达水平及CD8+CD2 8+/CD8+CD2 8- 均高于健康对照组 (P <0 0 1,P <0 0 5 )。 (2 )CAA肾阴虚患者CD2 8、CD8+CD2 8+表达水平及CD8+CD2 8+/CD8+CD2 8- 均高于肾阳虚患者 (P <0 0 1,P <0 0 5 )。结论 (1)CAA患者外周血共刺激分子CD2 8异常高表达 ,提示CD2 8失调可能在CAA免疫发病中起重要作用。 (2 )CAA患者外周血CD2 8、CD8+CD2 8+的表达水平及CD8+CD2 8+/CD8+CD2 8- 可以作为CAA辨证分型的参考指标 ,肾阴虚患者的免疫紊乱较肾阳虚患者严重。

再生障碍性贫血中医辨证分型的客观量化与临床意义

目的:应用统计学判别分析方法,筛选53项免疫学指标,建立再生障碍性贫血(aplastic anemia,AA)的中医证型判别方程,使AA中医证型客观量化。方法:采用流式细胞技术,对AA患者34例,健康对照人群34名外周血的免疫学指标进行检测,同时对AA患者进行辨证分型,以判别分析方法建立AA辨证分型的判别方程,对中医证型进行客观量化。结果:筛选出CD45RA+绝对值、CD3+CD25+绝对值、CD3+CD25+(%)、CD3+HLA-DR+绝对值和CD4+γδT(%)等5个最有意义免疫指标;建立AA中医证型的空间分布位置图;组成AA辨证分型的判别方程,对中医证候进行客观量化,其判别总正确率为76.5%。结论:应用判别分析方法建立了AA中医辨证各型判别方程,使AA辨证分型得以客观量化,具有临床实际意义。筛选出与辨证分型最相关的5个免疫学指标,与AA免疫学发病机制关系密切,说明AA中医辨证分型存在物质基础。

再生障碍性贫血患儿骨髓间充质干细胞体外生物学特性及其与免疫抑制疗效的关系

目的探讨再生障碍性贫血(再障)患儿骨髓间充质干细胞(MSC)体外生物学特性及与免疫抑制治疗(IST)疗效的关系,评价MSC异常在再障发生、发展中的作用。方法对29例再障患儿进行了骨髓MSC培养,其中17例患儿接受IST,观察MSC体外生长特点、表面标志、细胞周期、对PHA刺激的外周血淋巴细胞增殖的抑制作用,并与5例正常儿童骨髓作对照;观察再障患儿MSC异常与IST疗效的关系。结果55%(16/29)的再障患儿表现为不同程度的MSC生长异常,主要为MSC数量减少及增殖能力下降,其中以重型再障(SAA)、病程较长者或放/化疗后再障为多见。培养成功的再障患儿第3代MSC表面标志、细胞周期、转化生长因子-β1(TGF-β1)分泌水平及对PHA刺激的淋巴细胞增殖的抑制作用与对照组比较,差异均无显著性(P>0.05)。在17例接受IST患儿中,9例MSC生长基本正常的再障患儿经IST后8例达完全缓解,而8例MSC生长异常者仅2例达完全缓解,两组比较差异具有显著性(P<0.01)。结论多数再障患儿骨髓MSC体外生长存在不同程度的异常,其MSC异常对IST后患儿骨髓造血功能恢复具有一定的负面影响。

补肾法治疗慢性再生障碍性贫血的临床研究

目的:观察补肾法治疗慢性再生障碍性贫血的临床疗效。方法:收集2007年1月—2012年1月在浙江中医药大学附属第一医院的门诊及住院69例病人。将患者进行辨证分型,其中肾阳虚组(23例)、肾阴虚组(19例)、肾阴阳两虚组(27例),然后进行奇偶数字随机抽取,分为中医治疗组和西医治疗组,其中中医治疗组36例中肾阳虚组(12例)、肾阴虚组(10例)、肾阴阳两虚组(14例);西医组33例中肾阳虚组(11例)、肾阴虚组(9例)、肾阴阳两虚组(13例)。以3个月为1个疗程,通过2个疗程的治疗后观察患者中医证候、外周血象及骨髓象变化。结果:①中医组治疗慢性再障在改善中医证候方面与西医组比较,具有显著性差异(P<0.05)。②中医组治疗前后相比血红蛋白、白细胞计数、血小板计数、网织红细胞均有不同程度的升高,肾阳虚型中医组与西医组治疗后相比,外周血细胞增长优于西医组,两者有差异(P<0.05)。③中医组治疗慢性再障过程中的不良反应较西医组轻。结论:补肾法治疗慢性再生障碍性贫血能明显改善临床症状,提高临床疗效,降低药物不良反应,为中西医结合治疗慢性再障提供较好的治疗方案。

慢性再生障碍性贫血中医分型的相关因素分析

目的:探讨性别、发病年龄、病程、血细胞减少程度、既往药物治疗和机体免疫水平等因素与慢性再生障碍性贫血(CAA)中医辨证分型的关系。方法:采用回顾总结病史,并运用免疫比浊法和流式细胞仪技术检测37例肾阳虚证和23例肾阴虚证CAA患者血清补体C3、C4含量、免疫球蛋白(Ig)含量以及外周血(PB)T细胞亚群的表达水平,分析其与中医证型的关系。结果:①CAA肾阳虚和肾阴虚组患者的发病年龄、性别、病程、血细胞减少程度和既往用药均无差异。②两组血清C3、C4含量和T细胞亚群表达存在显著差异,前者C3、C4含量明显降低,后者CD8+细胞高表达且血清C3含量与PBCD8+细胞表达呈正相关(r=0·30),与CD4/CD8比值呈负相关(r=-0·31),P<0·05。两组Ig含量以及NK细胞表达均降低且无组间差异。结论:CAA中医辨证分型和免疫指标血清补体C3、C4含量和T细胞亚群CD4+、CD8+表达水平密切相关,但与患者的性别、发病年龄、病程、血细胞减少程度、既往用药无关。

再生障碍性贫血患者T细胞CD_(45)RA/RO表达与中医辨证分型的相关性

目的:应用统计学判别分析方法,建立再生障碍性贫血(AA)的中医辨证分型判别方程,探讨T细胞CD45RA/RO与辨证分型的关系。方法:采用流式细胞技术对34例AA患者及34例健康对照者外周血免疫学指标进行检测,同时对AA患者进行辨证分型。结果:筛选出CD45RA+绝对值等5个最有意义的免疫指标,组成AA辨证分型判别方程,其判别总正确率为76.5%。与健康对照组比较,CD8+CD45RO+(%)在AA辨证分型各组中显著上升(P<0.05或P<0.01)。结论:AA患者CD8+CD45RO+(%)表达显著增高,证实了患者体内T细胞异常活化后转化为记忆T细胞,进而导致骨髓衰竭的免疫学发病机制,说明中医辨证分型确有其客观物质基础。CD45RA+绝对值在辨证分型中变化显著,可作为AA中医辨证分型的一个客观指标。