Epstein-Barr virus-induced infection-associated hemophagocytic lymphohistiocytosis with acute liver injury:A case report

BACKGROUND Hemophagocytic lymphohistiocytosis(HLH)is a severe hyperinflammatory reaction,which is rare and life-threatening.According to the pathogen,HLH is divided into genetic and acquired.The most common form of acquired HLH is infection-associated HLH,of which Herpes viruses,particularly Epstein-Barr virus(EBV),are the leading infectious triggers.However,it is difficult to distinguish between simple infection with EBV and EBV-induced infectionassociated HLH since both can destroy the whole-body system,particularly the liver,thereby increasing the difficulty of diagnosis and treatment.CASE SUMMARY This paper elaborates a case about EBV-induced infection-associated HLH and acute liver injury,aiming to propose clinical guides for the early detection and treatment of patients with EBV-induced infection-associated HLH.The patient was categorized as acquired hemophagocytic syndrome in adults.After the ganciclovir antiviral treatment combined with meropenem antibacterial therapy and methylprednisolone inhibition to inflammatory response,gamma globulin enhanced immunotherapy,the patient recovered.CONCLUSION From the diagnosis and treatment of this patient,attention should be paid to routine EBV detection and a further comprehensive understanding of the disease as well as early recognition and early initiation are keys to patients’survival.

Hemophagocytic lymphohistiocytosis caused by primary Epstein-Barr virus in patient with Crohn's disease

We present a case of a 19-year-old man with a 6-year history of Crohn's disease(CD), previously treated with 6-mercaptopurine, who was admitted to our department for Epstein-Barr virus(EBV) infection and subsequently developed a hemophagocytic lymphohistiocytosis(HLH). HLH is a rare disease which causes phagocytosis of all bone marrow derived cells. It can be a primary form as a autosomic recessive disease, or a secondary form associated with a variety of infections; EBV is the most common, the one with poorer prognosis. The incidence of lymphoproliferative disorders was increased in patients with inflammatory bowel disease(IBD) treated with thiopurines. Specific EBV-related clinical and virological management should be considered when treating a patient with IBD with immunosuppressive therapy. Moreover EBV infection in immunosuppressed patient can occur with more aggressive forms such as encephalitis and diffuse large B cell lymphoma. Our case confirms what is described in the literature; patients with IBD, particularly patients with CD receiving thiopurine therapy, who present 5 d of fever and cervical lymphadenopathy or previous evidence of lymphopenia should be screened for HLH.

Treatment of Epstein-Barr virus-related hemophagocytic lymphohistiocytosis:Study protocol of a prospective pilot study

In this manuscript, a number of debatable issues related to the diagnosis and treatment of Epstein-Barr virus-related hemophagocytic lymphohistiocytosis(EBVHLH) will be addressed. Considering the heterogeneous nature of EBV-HLH, diagnostic efforts are required toclarify the precise nature of the disease at diagnosis, the number of EBV genome copies in peripheral blood, and localization of the EBV genome in lymphoid cells(B, T, or natural killer cells). Although the majority of cases of EBV-HLH develop without evidence of immunodeficiency, some cases have been found to be associated with chronic active EBV infection, genetic diseases such as X-linked lymphoproliferative disease(XLP, type 1, or type 2), or familial HLH(FHL, types 2-5). Due to such background heterogeneity, the therapeutic results of EBV-HLH have also been found to vary. Patients have been found to respond to corticosteroids alone or an etoposide-containing regimen, whereas other patients require hematopoietic stem cell transplantation. Thus, decision-making for optimal treatment of EBVHLH and its eventual outcome requires evaluation in consideration of the precise nature of the disease. A protocol for a pilot study on the treatment of patients with EBV-HLH is presented here.

Drug associated vanishing bile duct syndrome combined with hemophagocytic lymphohistiocytosis

A 28-year-old woman with untreated autoimmune disorder, demonstrated skin rash and fever after taking Amoxicillin-clavulanate and developed progressive jaundice. A bone marrow aspiration indicated an increased number of macrophages with hemophagocytosis and liver biopsy showed pure centrilobular cholestasis with necrosis and some absence of portal bile ducts. Furthermore, a serological test for Epstein-Barr virus was positive. Under treatment by liver dialysis and administration of steroids led to rapidly defervescence and clinical improvement. However, liver enzymes were still markedly elevated with persistent anemia, even after immunosuppressive treatment. The patient is currently waiting for liver transplantation. This is the ?rst description of vanishing bile duct syndrome combined with hemophagocytic lymphohistiocytosis, with underlying causes including infection, drug-induced factors and untreated autoimmune disorder.

Hemophagocytic lymphohistiocytosis: Recent progress in the pathogenesis, diagnosis and treatment

Hemophagocytic lymphohistiocytosis(HLH) is a hyperinflammatory syndrome that develops as a primary(familial/hereditary) or secondary(non-familial/hereditary) disease characterized in the majority of the cases by hereditary or acquired impaired cytotoxic T-cell(CTL) and natural killer responses. The molecular mechanisms underlying impaired immune homeostasis have been clarified, particularly for primary diseases. Familial HLH(familial hemophagocytic lymphohistiocytosis type 2-5, Chediak-Higashi syndrome, Griscelli syndrome type 2, Hermansky-Pudlak syndrome type 2) develops due to a defect in lytic granule exocytosis, impairment of(signaling lymphocytic activation molecule)-associated protein, which plays a key role in CTL activity [e.g., X-linked lymphoproliferative syndrome(XLP) 1], or impairment of X-linked inhibitor of apoptosis, a potent regulator of lymphocyte homeostasis(e.g., XLP2). The development of primary HLH is often triggered by infections, but not in all. Secondary HLH develops in association with infection, autoimmune diseases/rheumatological conditions and malignancy. The molecular mechanisms involved in secondary HLH cases remain unknown and the pathophysiology is not the same as primary HLH. For either primary or secondary HLH cases, immunosuppressive therapy should be given to control the hypercytokinemia with steroids, cyclosporine A, or intravenous immune globulin, and if primary HLH is diagnosed, immunochemotherapy with a regimen containing etoposide or anti-thymocyte globulin should be started. Thereafter, allogeneic hematopoietic stem-cell transplantation is recommended for primary HLH or secondary refractory disease(especially EBVHLH).

Epstein-Barr virus-associated hemophagocytic lymphohistiocytosis： a retrospective study of 78 pediatric cases in mainland of China

Background The clinical characteristics of Epstein-Barr virus-associated hemophagocytic lymphohistiocytosis （EBV-HLH） are largely unreported in the pediatric patients in mainland of China. The main aim of this study was to recognize the clinical features of EBV-HLH in children and to explore its prognosis and risk factors. Methods A retrospective study was performed on 78 pediatric patients with EBV-HLH who were admitted to Beijing Children＇s Hospital between 2003 and 2008. All patients＇ medical records were reviewed and analyzed. For each patient, demographic, clinical, laboratory and outcome information was collected. Statistical analysis was conducted via multivariate and univariate analysis. Results The age of onset peaked between 1-2 years and boys were more likely developed EBV-HLH. EBV-HLH occurred mainly in the serological pattern with EBV nuclear antigen （EBNA） positive （70.5%）. The overall fatality of the disease was 56.7%. Twelve of the 39 fatalities （30.8%） died rapidly within 2 months after diagnosis. Multivariate analysis revealed that not receiving chemotherapy （P=0.002）, 〉4 weeks of illness prior to diagnosis （P=0.004）, and albumin levels 〈20 g/L （P=-0.045） significantly predicted an increased fatality risk. Conclusions EBV-HLH is a severe disease with a high fatality rate that occurs mainly in the serological pattern with EBNA positive. Early initiation of chemotherapy and timely diagnosis significantly improves survival rate. Practical strategies should focus on reducing the likelihood of early death.

Epstein-Barr virus associated secondary hemophagocytic lymphohistiocytosis with an unusual presentation of abdominal compartment syndrome

Hemophagocytic lymphohistiocytosis(HLH)is a cytokine storm syndrome caused by an overactive but ineffective immune reaction.Without prompt diagnosis and treatment,HLH is life-threatening.However,presenting symptoms are often nonspecific,with fatigue and fever being the most common.A high index of suspicion is therefore critical for early diagnosis and timely management.A previously healthy,65-year-old female who initially presented with fever and abdominal pain developed abdominal compartment syndrome(ACS)requiring decompressive laparotomy on hospital day 6.Intraoperative frozen sections of biopsied liver showed intense portal lymphohistiocytic infiltrates.Epstein-Barr virus DNA copy numbers escalated from 600 copies/mL after admission to 134,000 copies/mL before death.The diagnostic criteria of HLH-2004 were met.Patient expired on hospital day 12.It is important to raise awareness of ACS being an unusual presentation of HLH.Recent changes in diagnostic criteria tailored to adult HLH cases are reviewed.

化疗联合亲缘HLA半相合淋巴细胞输注治疗难治性成人EBV相关噬血细胞综合征

目的观察化疗联合亲缘HLA半相合淋巴细胞输注治疗难治性成人EB病毒相关噬血细胞综合征(EBV-HLH)的疗效。方法回顾性收集2017年7月至2019年7月于首都医科大学附属北京友谊医院经过噬血细胞综合征一线方案(HLH-94/HLH-04)及挽救方案(DEP/L-DEP)治疗均无效后通过化疗联合亲缘HLA半相合淋巴细胞输注治疗的16例难治性成人EBV-HLH患者的临床资料。亲缘HLA半相合淋巴细胞输注方案为:在DEP方案化疗后24 h输注亲缘HLA半相合淋巴细胞(阿霉素脂质体25 mg/m^2第一天;依托泊苷100 mg/m^2第一天;甲基强的松龙15 mg/kg第一天,淋巴细胞输注第三天)。取化疗前1天及淋巴细胞输注后3天的化验结果进行比较(包括血象、肝功能、铁蛋白、EBV-DNA拷贝数等)。结果16例在经过一线治疗及挽救治疗后仍未达到部分应答的患者中,经过化疗联合亲缘HLA半相合淋巴细胞输注后的5例患者达到了部分应答,11例患者仍为无应答。在5例达到了部分应答的患者中3例患者进行了异基因造血干细胞移植。回输后的患者血小板得到一定程度的恢复,铁蛋白和EBV-DNA的拷贝数存在下降的趋势。结论对于经过噬血细胞综合征一线方案(HLH-94/HLH-04)及挽救方案(DEP/L-DEP)治疗均无效,并且无法立即接受异基因造血干细胞移植的EBV-HLH患者,化疗联合亲缘HLA半相合淋巴细胞输注的方法可作为尝试,它可以使部分患者拥有异基因造血干细胞移植的机会,对控制疾病的进展有一定作用。

儿童EB病毒感染非肿瘤性疾病与病毒潜伏期膜蛋白基因多态性的相关性研究

目的分析儿童EB病毒(EBV)感染相关非肿瘤性疾病与病毒潜伏期膜蛋白(LMP1)基因多态性的相关性。方法选择2017年12月至2020年12月在我院确诊的94例EBV感染相关非肿瘤性疾病患儿为观察组,其中传染性单核细胞增多症(IM)40例,EBV相关噬血细胞性淋巴组织细胞增生症(EBV-HLH)30例,慢性活动性EBV感染(CAEBV)24例,随机选取同期携带EBV病毒的无症状儿童94例为对照组。检测所有对象血清免疫球蛋白水平,RT-PCR检测外周血淋巴细胞EBV DNA载量和LMP1 mRNA水平,Westernblot检测LMP1蛋白表达,巢式PCR检测LMP1基因多态性。Pearson相关性分析LMP1基因多态性与病毒载量、LMP1表达和免疫球蛋白之间的关系。结果IM组患儿血清IgA和IgM水平高于对照组,EBV-DNA载量和LMP1表达水平高于对照组(P<0.05);EBV-HLH组IgG、IgA、IgM、C3和C4水平低于IM组和对照组(P<0.05),EBV-DNA载量和LMP1表达水平高于IM组和对照组(P<0.05);CAEBV组患儿IgG、IgA、C3和C4水平低于IM组和对照组,高于EBV-HLH组(P<0.05),IgM和IgE水平高于EBV-HLH组、IM组和对照组(P<0.05),EBV-DNA载量和LMP1表达水平低于EBV-HLH组,高于IM组和对照组(P<0.05);EBV-HLH组患儿LMP1基因XhoⅠ位点(-)和del-LMP1的发生率明显高于IM组和对照组(P<0.05)。Pearson相关性分析显示,EBV感染相关非肿瘤疾病患儿LMP1基因XhoⅠ位点(-)变异和del-LMP1位点变异与EBV-DNA和LMP1表达呈显著正相关关系(P<0.05)。结论EBV感染相关非肿瘤疾病患儿LMP1基因XhoⅠ位点(-)变异和del-LMP1位点变异与疾病进展有关。

CD4^+CD25^+CD127^-调节性T细胞在小儿EB病毒相关噬血细胞综合征发病作用中的研究

目的:观察EB病毒(EBV)相关噬血细胞淋巴组织细胞增生症(EBV-HLH)患儿外周血CD4^+CD25^+CD127^-调节性T细胞(CD4^+CD25^+CD127^-Treg)亚群的含量,对比EBV-HLH患儿与同期来院体检的健康儿童的不同,了解EBV-HLH患儿的免疫状态,以探讨CD4^+CD25^+CD127^-Treg细胞在小儿EBV-HLH免疫中的意义。方法:建立流式细胞术检测外周血CD4^+CD25^+CD127^-Treg细胞的含量,检测30例EBV-HLH初诊患儿及30例同期来院体检的健康儿童的外周血CD4^+CD25^+Treg细胞数量。结果:EBV-HLH初诊组与正常对照组外周血CD4^+CD25^+CD127^-占CD4^+T细胞的比例分别为(3.65±1.12)%和(6.90±1.16)%,EBV-HLH初诊患儿组低于正常对照组,差异有统计学意义(P<0.05)。结论:EBV相关HLH患儿外周血中CD4^+CD25^+CD127^-Treg数量减低,表明EBV-HLH患儿免疫功能处于失衡状态。Treg细胞可能在EBV相关HLH的发生、发展中起一定作用,参与细胞免疫的调节可能是Treg细胞在EBV相关HLH免疫中的一个环节。

儿童EB病毒相关噬血细胞性淋巴组织细胞增生症诊疗进展

噬血细胞性淋巴组织细胞增生症（HLH）是一类多器官、多系统受累的临床综合征，以持续发热、脾大、血细胞减少、高三酰甘油血症和低纤维蛋白原血症为主要表现。该病发病急、病情进展迅速、病死率高，是儿科疾病中的危重症。EB病毒（EBV）相关HLH（EBV-HLH）是HLH中最重要的类型，同时也是EBV感染的严重并发症，在血液病及感染专业均有深入的研究，现主要阐述儿童EBV—HLH的诊断和治疗方面的研究进展。

成人EB病毒相关噬血细胞综合征的危险因素

目的分析成人EB病毒(EBV)感染导致的传染性单核细胞增多症(IM)和EBV相关噬血综合征(EBV-HLH)患者临床特征,探讨IM发展为EBV-HLH的危险因素。方法收集重庆医科大学附属第一医院2016年1月至2020年12月收治的217例EBV感染者,按照是否发生噬血分为IM组和EBV-HLH组,回顾性收集和分析两组患者的一般资料、临床表现、实验室检查、治疗及预后特点,采用二元Logistic回归分析IM进展为EBV-HLH的危险因素。结果EBV-HLH组患者中位发病年龄显著大于IM组[25(21,56)岁vs.21(18,25)岁,Z=-2.658、P=0.008],IM组患者较EBV-HLH组更易出现扁桃体炎[83.1%(167/201)vs.25.0%(4/16),χ^(2)=26.556、P<0.001];而EBV-HLH组患者较IM组热峰更高[40.3(39.8,40.9)℃vs.38.9(38.4,39.3)℃,Z=-5.723、P<0.001]、热程更长[30(18,44)d vs.7(4,12)d,Z=-5.469、P<0.001],且更常见肝肿大、腹泻、黄疸、肺炎、出血(χ^(2)=18.341、13.444、27.344、68.405、32.967,P均<0.001)、心力衰竭(Fisher’s确切概率法:P=0.005)等表现,差异均有统计学意义。与IM组相比,EBV-HLH组患者血常规指标中白细胞[2.2(1.4,3.0)×10^(9)/L vs.11.2(7.7,14.4)×10^(9)/L,Z=-5.883、P<0.001]、血红蛋白[(87.8±17.1)g/L vs.(134.4±16.5)g/L,t=-10.806、P<0.001]、血小板[45.5(27.0,74.5)×10^(9)/L vs.165.0(133.0,205.5)×10^(9)/L,Z=-6.316、P<0.001]均显著降低;肝功能指标总胆红素[58.2(13.9,108.3)μmol/L vs.12.3(9.1,16.7)μmol/L,Z=-4.119、P<0.001]、乳酸脱氢酶[3000.0(953.8,6665.8)U/L vs.1459.5(991.0,2023.6),Z=-3.206、P=0.001]显著升高,白蛋白[(26.9±4.6)g/L vs.(40.1±4.6)g/L,t=-11.054、P<0.001]显著下降;凝血功能提示D-二聚体[4.8(0.8,10.4)mg/L vs.1.0(0.7,1.7)mg/L,Z=-3.063、P=0.002]显著升高,纤维蛋白原[0.9(0.7,2.9)g/L vs.2.7(2.2,3.1)g/L,Z=-3.395、P=0.001]显著下降,差异均有统计学意义。EBV-HLH组患者较IM组患者C-反应蛋白[51.7(31.6,90.0)mg/L vs.17.2(7.1,23.0)mg/L,Z=-3.206、P<0.001]、铁蛋白[7835.0(2101.5,23481.5)ng/mL vs.563.3(213.9,1215.5)ng/ml,Z=-4.859、P=0.001]、甘油三酯[2.5(1.8,2.9)mmol/L vs.1.6(1.1,2.2)mmol/L,Z=-2.809、P=0.005]均显著升高,差异均有统计学意义。EBV-HLH组患者CD4^(+)T百分比[36.28(28.90,46.02)%vs.13.07(9.49,18.16)%,Z=-4.698、P<0.001]、B细胞百分比[6.50(1.36,9.74)%vs.1.89(1.06,4.05)%,Z=-2.217、P=0.027]较IM组升高,CD3^(+)T细胞百分比[80.14(70.17,87.59)%vs.91.71(89.02,94.40)%,Z=-3.750、P<0.001]、CD8^(+)T细胞百分比[35.60(23.58,50.98)%vs.72.98(65.02,80.00)%,Z=-4.938、P<0.001]以及所有淋巴细胞亚群计数均较IM组显著下降,差异均有统计学意义。二元Logistic多因素回归分析发现:发热天数(OR=1.171、95%CI:1.010~1.357、P=0.036)为影响IM发展为EBV-HLH的独立危险因素。结论EBV感染引起的IM患者有持续发热表现、伴多系血细胞下降和器官功能损伤者,应完善噬血细胞综合征筛查,尽早予以治疗以期改善预后。

血浆及全血EB病毒DNA对EB病毒相关噬血细胞性淋巴组织细胞增生症患儿预后的影响

目的探讨血浆及全血EB病毒(EBV)DNA水平对EBV相关噬血细胞性淋巴组织细胞增生症(EBV-HLH)患儿预后的影响。方法对2016年1月至2017年12月首都医科大学附属北京儿童医院血液肿瘤中心收治的66例EBV-HLH患儿的临床资料进行回顾性分析,包括入院时、治疗2周、治疗4周血浆及全血EBV-DNA的动态改变,并根据EBV-DNA的拷贝数将血浆EBV-DNA分为阳性组和阴性组,利用受试者工作特征曲线(ROC)将全血EBV-DNA分为高水平组及低水平组;采用χ2检验比较不同水平患儿之间预后不良发生率,Log-Rank检验评估无事件生存情况来分析其预后意义。结果单因素分析结果显示,入院时血浆或全血EBV-DNA水平对EBV-HLH预后影响不大,治疗2周及4周血浆EBV-DNA阳性(≥500拷贝/mL)或全血EBV-DNA载量>(5.04~5.09)×105拷贝/mL是影响患儿预后及无进展生存的重要因素(P<0.001)。此外中枢神经系统受累(P=0.025)、白细胞(WBC)减少(WBC≤3×109/L,P=0.031)、中性粒细胞(ANC)缺乏(ANC≤0.5×109/L,P=0.041)、血红蛋白(Hb)降低(Hb≤90 g/L,P=0.023)及清蛋白减少(≤26 g/L,P=0.012),提示也具有一定预后意义。Cox回归多因素分析显示,仅治疗4周时血浆EBV-DNA载量与中枢神经系统累及是独立预后因素(风险比率=7.139,P=0.032;风险比率=6.455;P=0.042),而不同时间点的全血及治疗2周时血浆EBV-DNA水平的预后价值较低。结论 EVB-HLH患儿治疗4周血浆EBV-DNA水平可作为早期判断病情、尽早识别预后不良的客观指标,能更好地指导EBV-HLH的治疗。

人类疱疹病毒4型相关噬血细胞综合征早期预后的危险因素分析

目的探讨影响人类疱疹病毒4型相关噬血细胞综合征(EBV-HLH)早期预后的危险因素。方法本研究为回顾性研究,选取2015年1月至2020年12月西安市儿童医院感染三科收治的30例EBV-HLH患儿,男15例,女15例,年龄(3.5±2.6)岁,年龄范围为8个月29 d~11岁1个月。根据早期预后(发病30 d结局)分为存活组与病死组,存活组患儿23例,病死组患儿7例。收集比较两组患儿的年龄、性别、最高体温、中性粒细胞计数、血小板计数、血红蛋白、总胆红素、谷丙转氨酶(ALT)、谷草转氨酶(AST)、乳酸脱氢酶(LDH)、白蛋白、甘油三酯、血清铁蛋白、血浆人类疱疹病毒4型脱氧核糖核酸定量(EBV-DNA)水平及消化道出血、肝功能衰竭、浆膜腔积液、支气管肺炎发生率。选取单因素分析差异有统计学意义的指标,进一步纳入二元非条件logistic回归分析,分析影响EBV-HLH患儿早期预后的独立危险因素,采用受试者操作特征(ROC)曲线选取其最佳截断值。结果对病死组和存活组的观察指标进行分析,两组患儿的年龄、性别、最高体温、血小板计数、血红蛋白、总胆红素、甘油三酯、血清铁蛋白、EBV-DNA水平,及消化道出血、肝功能衰竭、浆膜腔积液、支气管肺炎发生率比较,差异无统计学意义(P>0.05)。存活组患儿的中性粒细胞计数[(0.61±0.34)×10^(9)/L]、白蛋白[30.4(26.2,34.2)g/L]、纤维蛋白原[(1.26±0.56)g/L]水平高于病死组[(0.31±0.26)×10^(9)/L、24.0(22.1,27.0)g/L、(0.68±0.37)g/L],ALT[171(105,312)g/L]、AST[351(199,758)U/L]、LDH[1929(1081,2868)U/L]水平低于病死组[559(318,894)g/L、2319(1268,3556)U/L、10750(3500,13178)U/L],差异有统计学意义(P<0.05)。对单因素分析中差异有统计学意义的指标进行二元非条件logistic回归分析。进入回归模型的变量有2个,分别是AST水平[OR=1.001,95%CI(1.001~1.002)]、中性粒细胞计数[OR=0.001,95%CI(0~0.501)]。采用ROC曲线对AST水平、中性粒细胞计数进行最佳截断值测定。结果显示,AST水平的曲线下面积是0.919(95%CI为0.814~1.000),中性粒细胞计数的曲线下面积是0.773(95%CI为0.585~0.961)。AST水平、中性粒细胞计数的截断值分别为1224.500 U/L、0.285×10^(9)/L时,约登指数最大,其灵敏度分别为85.7%、87.0%,特异度分别为91.3%、57.1%。结论EBV-HLH早期病死率高,AST≥1224.5 U/L、中性粒细胞计数≤0.285×10^(9)/L提示早期预后不佳。在疾病早期识别出可能预后不佳的患儿,从而开展个体化的分层治疗,对EBV-HLH患者的治疗具有重大意义。