Microbiology laboratory and the management of motherchild varicella-zoster virus infection

Varicella-zoster virus, which is responsible for varicella(chickenpox) and herpes zoster(shingles), is ubiquitous and causes an acute infection among children, especially those aged less than six years. As 90% of adults have had varicella in childhood, it is unusual to encounter an infected pregnant woman but, if the disease does appear, it can lead to complications for both the mother and fetus or newborn. The major maternal complications include pneumonia, which can lead to death if not treated. If the virus passes to the fetus, congenital varicella syndrome, neonatal varicella(particularly serious if maternal rash appears in the days immediately before or after childbirth) or herpes zoster in the early years of life may occur depending on the time of infection. A Microbiology laboratory can help in the diagnosis and management of mother-child infection at four main times:(1) when a pregnant woman has been exposed to varicella or herpes zoster, a prompt search for specific antibodies can determine whether she is susceptible to, or protected against infection;(2) when a pregnant woman develops clinical symptoms consistent with varicella, the diagnosis is usually clinical, but a laboratory can be crucial if the symptoms are doubtful or otherwise unclear(atypical patterns in immunocompromised subjects, patients with post-vaccination varicella, or subjects who have received immunoglobulins), or if there is a need for a differential diagnosis between varicella and other types of dermatoses with vesicle formation;(3) when a prenatal diagnosis of uterine infection is required in order to detect cases of congenital varicella syndrome after the onset of varicella in the mother; and(4) when the baby is born and it is necessary to confirm a diagnosis of varicella(and its complications), make a differential diagnosis between varicella and other diseases with similar symptoms, or confirm a causal relationship between maternal varicella and malformations in a newborn.

Review of varicella-zoster virus infections in pregnant women and neonates

Even though varicella is rare in pregnancy, the disease can lead occasionally to disastrous illnesses for both the mother and her neonate. By contrast, normal zoster is not associated with special problems during pregnancy and peri- natal period. Pregnant women, who contract varicella, are at risk of varicella pneumonia which must be regarded as medical emergency. At any stage during pregnancy, chickenpox may cause intrauterine infection. The consequences for the fetus depend on the time of maternal disease. During the first two trimesters, maternal varicella may result in congenital varicella syndrome which may occur in nearly 2%. Typical symptoms are skin lesions in dermatomal distribution, neurological defects, eye diseases, and skeletal anomalies. Maternal infection near term is associated with a substantial risk of intrauterine acquired neonatal chickenpox in the neonate. If the mother develops varicella rash between day 4 (5) ante partum and day 2 post partum, generalized neonatal varicella leading to death in about 20% of the cases has to be expected. The present paper reviews the clinical consequences and the currently available concepts of prevention, diagnosis, and therapy of varicella-zoster virus infections during pregnancy.

Varicella-zoster virus meningitis after spinal anesthesia:A case report

BACKGROUND Headache is a common complication of regional anesthesia.The treatment of post spinal anesthesia headache varies depending on the cause.Although meningitis is rare,it can cause significant harm to the patient.Post dural puncture headache and septic meningitis are the most commonly suspected causes of post spinal anesthesia headache;however,other causes should also be considered.CASE SUMMARY A 69-year-old woman was scheduled for varicose vein stripping surgery under spinal anesthesia.The procedure was performed aseptically,and surgery was completed without any complications.After 4 d,the patient visited the emergency room with complaints of headache,nausea,and anorexia.Clinical examination revealed that the patient was afebrile.Considering the history of spinal anesthesia,post dural puncture headache and septic meningitis was initially suspected,and the patient was treated with empirical antibiotics.Subsequently,varicella-zoster virus PCR test result was positive,and all other test results were negative.The patient was diagnosed with meningitis caused by varicella-zoster virus and was treated with acyclovir for 5 d.The headache improved,and the patient was discharged without any problems.CONCLUSION Viral meningitis due to virus reactivation may cause headache after regional anesthesia.Therefore,clinicians should consider multiple etiologies of headache.

Varicella zoster virus vaccines: potential complications and possible improvements

Varicella zoster virus(VZV) is the causative agent of varicella(chicken pox) and herpes zoster(shingles). After primary infection, the virus remains latent in sensory ganglia, and reactivates upon weakening of the cellular immune system due to various conditions, erupting from sensory neurons and infecting the corresponding skin tissue. The current varicella vaccine(v-Oka) is highly attenuated in the skin, yet retains its neurovirulence and may reactivate and damage sensory neurons. The reactivation is sometimes associated with postherpetic neuralgia(PHN), a severe pain along the affected sensory nerves that can linger for years, even after the herpetic rash resolves. In addition to the older population that develops a secondary infection resulting in herpes zoster, childhood breakthrough herpes zoster affects a small population of vaccinated children. There is a great need for a neuro-attenuated vaccine that would prevent not only the varicella manifestation, but, more importantly, any establishment of latency, and therefore herpes zoster. The development of a genetically-defined live-attenuated VZV vaccine that prevents neuronal and latent infection, in addition to primary varicella, is imperative for eventual eradication of VZV, and, if fully understood, has vast implications for many related herpesviruses and other viruses with similar pathogenic mechanisms.

Detection of Varicella Zoster Virus DNA within Lesions and Healed Skin Lesions of Herpes Zoster by PCR

Varicella zoster virus(VZV) DNA in blister lesions and skin biopsies obtained from healed skin lesions in 16 patients with herpes zoster was detected using polymerase chain reaction. A 385 bp VZV DNA fragment was found in all the blister lesions and in two of six biopsies from the skin lesions healed within two months by PCR. No VZV DNA was found in the skin lesions more than two months after healing in 10 cases of herpes zoster. VZV DNA may be detected at the sites of resolved herpes zoster lesions within short duration.

Transverse myelitis after infection with varicella zoster virus in patient with normal immunity: A case report

BACKGROUND Varicella zoster virus(VZV)is a human neurotropic and double-stranded DNA alpha-herpes virus.Primary infection with VZV usually occurs during childhood,manifesting as chickenpox.Reactivation of latent VZV can lead to various neurological complications,including transverse myelitis(TM);although cases of the latter are very rare,particularly in newly active VZV infection.CASE SUMMARY We report here an unusual case of TM in a middle-aged adult immunocompetent patient that developed concomitant to an active VZV infection.The 46-year-old male presented with painful vesicular eruption on his left chest that had steadily progressed to involvement of his back over a 3-d period.Cerebrospinal fluid testing was denied,but findings from magnetic resonance imaging and collective symptomology indicated TM.He was administered antiviral drugs and corticosteroids immediately but his symptom improvement waxed and waned,necessitating multiple hospital admissions.After about a month of repeated treatments,he was deemed sufficiently improved for hospital discharge to home.CONCLUSION VZV myelitis should be suspected when a patient visits the outpatient pain clinic with herpes zoster showing neurological symptoms.

中枢神经系统水痘-带状疱疹病毒感染的临床表型分析

目的水痘-带状疱疹病毒(varicella-zoster virus,VZV)是中枢神经系统(central nervous system,CNS)病毒感染的常见病因,其临床表现多样,总结分析其临床表现、转归,有助于早期识别,指导治疗,判断预后。方法回顾2014—2021年北京协和医院神经科诊治的11例中枢神经系统VZV感染病例,分析临床特点、预后,采用改良Rankin评分(modified Rankin scale,mRS)评估。结果男性7例(63.63%),女性4例(36.36%)。临床类型包括脑膜炎4例(36.36%),边缘性脑炎3例(27.27%),血管炎3例(27.27%),脊髓炎1例(9.09%),3例患者伴有皮肤带状疱疹(27.27%),脑脊液(cerebrospinal fluid,CSF)压力165(85,330)mmH2O,脑脊液白细胞数46(9,471)×106/L,脑脊液蛋白0.85(0.32,3.12)g/L,脑脊液葡萄糖3.0(2.5,4.0)mmol/L。治疗前、后mRS评分分别为3(1,5)分与0(0,6)分,差异具有统计学意义(P<0.05)。结论中枢神经系统VZV的主要临床类型包括脑膜炎、边缘性脑炎,脑血管炎与脊髓炎等,其中以脑膜炎型预后良好,免疫抑制状态患者发生VZV脑血管炎的预后较差。脑脊液mNGS是中枢神经系统VZV感染重要的确诊实验。

Varicella zoster meningitis complicating combined anti-tumor necrosis factor and corticosteroid therapy in Crohn's disease

Opportunistic viral infections are a well-recognized complication of anti-tumor necrosis factor (TNF) therapy for inflammatory bowel disease (IBD). Cases of severe or atypical varicella zoster virus infection, both primary and latent reactivation, have been described in association with immunosuppression of Crohn's disease (CD) patients. However, central nervous system varicella zoster virus infections have been rarely described, and there are no previous reports of varicella zoster virus meningitis associated with anti-TNF therapy among the CD population. Here, we present the case of a 40-year-old male with severe ileocecal-CD who developed a reactivation of dermatomal herpes zoster after treatment with prednisone and adalimumab. The reactivation presented as debilitating varicella zoster virus meningitis, which was not completely resolved despite aggressive antiviral therapy with prolonged intravenous acyclovir and subsequent oral valacyclovir. This is the first reported case of opportunistic central nervous system varicella zoster infection complicating anti-TNF therapy in the CD population. This paper also reviews the literature on varicella zoster virus infections of immunosuppressed IBD patients and the importance of vaccination prior to initiation of anti-TNF therapy.

成人中枢神经系统水痘-带状疱疹病毒感染七例并文献复习

目的探讨成人中枢神经系统水痘-带状疱疹病毒(varicella-zoster virus,VZV)感染的临床特点及预后。方法选取2013年7月至2024年4月首都医科大学附属北京友谊医院的中枢神经系统VZV患者,收集患者的一般资料和临床资料,分析患者的临床特点及预后,并复习既往文献。结果共纳入7例患者,其中男6例、女1例;发病年龄35~94岁,平均65.1岁。7例均为急性或亚急性起病、伴发热,4例伴意识障碍,5例脑膜刺激征(+),4例伴肢体瘫痪、头痛、头晕,3例伴周围性面瘫,5例伴皮肤疱疹。脑脊液压力80~190 mmH2O(1 mmH2O=0.0098 kPa)、WBC 14~1039×106/L、蛋白40.38~444.43 mg/dl、葡萄糖2.34~6.01 mmol/L、氯化物108.90~125.00 mmol/L。脑脊液宏基因二代测序(metage⁃nomic next-generation sequencing,mNGS)检测的VZV病毒DNA序列数7~8869。影像学结果示脑干及小脑受累3例,颈髓受累1例,硬脑膜或脊膜强化3例,伴硬膜下积液或出血1例、伴急性脑梗死2例。治疗后,住院期间死亡1例(发病后4个月),好转出院6例;死亡2例(发病后1.5~10个月),好转4例(发病后6~63个月)。既往文献报道,成人中枢神经系统VZV感染患者有病情重、预后差,脑脊液葡萄糖降低、合并颅神经或周围神经或脑血管受累等表现,但未见合并硬脑膜强化的病例报道。结论成人中枢神经系统VZV感染患者年龄分布较广、青年至高龄老年均可见,脑脊液蛋白和WBC可明显升高,部分患者葡萄糖和氯化物降低,类似结核杆菌感染。脑膜脑实质多同时受累时病情危重,高龄者预后差。怀疑中枢神经系统VZV感染者应尽早完善腰穿、脑脊液mNGS等辅助检查,在早期诊断和治疗后规范应用抗病毒感染药物,以改善预后。

水痘-带状疱疹病毒脑膜炎/脑膜脑炎患者临床特征及预后因素分析

目的分析水痘-带状疱疹病毒(VZV)脑膜炎/脑膜脑炎患者临床特征以及预后的影响因素。方法选取2018年7月至2022年7月VZV脑膜炎/脑膜脑炎患者74例,分析患者临床资料,包括基本信息、合并疾病、疱疹部位、临床症状、脑脊液检测、影像学表现、疱疹出现神经系统症状时间、药物治疗开始时间及预后。结果发热、头痛、颅神经受损/急性认知改变、脑膜刺激征/恶心呕吐、RHS为VZV脑膜炎/脑膜脑炎常见的症状;头颅磁共振检查无特异表现;与VZV脑膜脑炎相比,VZV脑膜炎患者年龄较轻(P=0.008),脑脊液糖含量更低(P=0.02),患者出院时预后更好(P<0.001)。男性、出现神经系统症状至抗病毒药物治疗间隔时间>1.5 d是VZV脑膜炎/脑膜脑炎患者预后不良的独立危险因素。结论早期静脉应用抗病毒药物治疗VZV脑膜炎/脑膜脑炎预后良好,男性、出现神经系统症状至抗病毒药物治疗间隔时间>1.5d预后越差。

成人水痘-带状疱疹病毒相关颅内感染5例临床分析

目的探讨水痘-带状疱疹病毒(varicella zoster virus,VZV)相关颅内感染的临床特点,脑脊液及影像学表现,治疗及转归,为临床诊治提供参考。方法回顾性总结2019年4月至2023年4月临沂市人民医院神经内科收治的5例VZV患者的临床资料,对其临床表现、辅助检查、治疗及预后进行分析。结果5例VZV相关颅内感染患者男性多于女性,年龄(53.6±10.9)岁,急性起病,均有前驱感染病史。临床表现均有头痛、发热和局灶神经功能障碍。影像学检查可无明显异常或脑实质受累,脑实质受累时病灶累及幕上及幕下,可合并出血。脑脊液检查表现为5例白细胞增高[(399.4±84.20)×10^(6)/L],4例氯化物降低[(107.65±7.17)mmol/L],5例蛋白含量均明显升高[(2.85±1.33)g/L],4例脑脊液糖/血糖<0.6,(0.52±0.05)。5例患者均通过脑脊液宏基因组二代测序(metagenomics next-generation sequencing,mNGS)检查确诊。抗病毒治疗整体预后良好。结论VZV颅内感染中老年起病,趋于年轻化。临床症状轻重取决于感染是否累及脑实质。脑脊液与结核性脑膜炎脑脊液表现类似。mNGS检测可提高鉴别敏感性、准确性。及早对因对症治疗大多数患者预后相对良好。

Regulation of Wnt/β-catenin signaling by herpesviruses

The Wnt/β-catenin signaling pathway is instrumental in successful differentiation and proliferation of mammalian cells. It is therefore not surprising that the herpesvirus family has developed mechanisms to interact with and manipulate this pathway. Successful coexistence with the host requires that herpesviruses establish a lifelong infection that includes periods of latency and reactivation or persistence. Many herpesviruses establish latency in progenitor cells and viral reactivation is linked to host-cell proliferation and differentiation status. Importantly, Wnt/β-catenin is tightly connected to stem/progenitor cell maintenance and differentiation. Numerous studies have linked Wnt/β-catenin signaling to a variety of cancers, emphasizing the importance of Wnt/β-catenin pathways in development, tissue homeostasis and disease. This review details how the alpha-, beta-, and gammaherpesviruses interact and manipulate the Wnt/β-catenin pathway to promote a virus-centric agenda.

迷迭香酸体外抗水痘-带状疱疹病毒的作用及其机制研究

目的研究迷迭香酸(RosA)体外抗水痘-带状疱疹病毒(VZV)的作用及其机制。方法采用不同浓度的RosA(400、200、100、50μmol/L)处理VZV感染的Vero细胞,采用细胞病变效应(CPE)法和MTT法评价RosA体外抗VZV的作用以及对细胞的毒性,采用RT-qPCR法检测RosA对VZV ORF36 mRNA表达的影响。结果当RosA浓度为100、200、400μmol/L时,RosA对VZV的抑制率分别为55.88%、78.99%和98.19%,其抑制效果与RosA浓度呈正比。当RosA浓度为400μmol/L时,RosA对VZV的灭活率为85.44%,灭活作用的EC_(50)为185.95μmol/L,RosA的CC 50为2362.10μmol/L,EC_(50)为63.02μmol/L,SI为37.48。当RosA浓度为100、200、400μmol/L时,VZV ORF36 mRNA的表达量分别下调了48.2%、85.9%、97.2%。结论RosA在体外具有抗VZV的作用,其抗病毒作用与RosA抑制VZV ORF36的转录有关。

水痘-带状疱疹病毒性脊髓神经根炎的临床特征分析

目的探讨水痘-带状疱疹病毒性脊髓神经根炎(varicella-zoster virus myeloradiculitis,VZVM)的临床特征。方法选择2016年6月—2021年6月作者医院收治确诊的8例VZVM,分析其临床表现、影像学、肌电图、脑脊液病原学基因检测、治疗及预后等。结果8例中男5例、女3例,发病年龄56~80岁,中位数(四分位数)59.5(57.0,60.0)岁。患者均急性起病,病程5~90 d,病程中位数(四分位数)15.5(14.0,17.0)d。8例患者发病前均有皮肤疱疹病史,出现皮肤疱疹至发生脊髓病变潜伏期1~36 d,中位数(四分位数)11.5(10.0,13.0)d。7例患者以疼痛起病,肢体无力8例,肢体麻木6例,尿便失禁6例;表现为脊髓横贯性损害6例,脊髓局灶性损害2例。7例患者行肌电图检查,其中4例可见脊髓病变相应神经支配区肌电图自发电位。5例患者行脑脊液和(或)血液病毒基因检测,其中3例均行血和脑脊液PCR疱疹病毒基因检测,2例均阳性,1例均阴性;2例行脑脊液微生物二代测序(mNGS),1例检测到VZV基因。8例脊椎MRI均表现为脊髓、神经根、神经节异常强化,病变仅累及颈段3例、胸段2例,同时累及颈、胸段2例,同时累及胸、腰段1例;8例均有髓内强化,4例呈髓内环形强化,2例髓内呈片状强化、2例髓内呈结节状强化;髓内长节段病变4例,其中累及颈、胸段各1例,累及颈-胸段,胸-腰段各1例。8例均应用阿昔洛韦和糖皮质激素治疗,5例症状基本恢复正常,2例遗留截瘫,1例病灶发展至延髓后死亡。结论VZVM常以疼痛起病,增强MRI可见神经根及脊髓异常强化,肌电图可检测到脊髓神经根病变支配区肌肉自发电位,脑脊液病毒基因测序可检测到VZV病毒可明确诊断。通过多种诊断方法,尽早明确诊断、早期抗病毒和适量激素治疗对改善预后十分重要。

某部新入伍人员水痘-带状疱疹病毒抗体血清学分析

目的了解某部新入伍人员的水痘免疫状况及抗体阳性率,为军队人员疫苗防控政策提供流行病学数据。方法采用整群抽样法对903名新入伍人员基本信息进行收集并分析,采集静脉血进行血清分离,采用水痘-带状疱疹病毒(VZV)IgG抗体ELISA试剂盒进行检测。结果903名入选的新入伍人员中,有198名曾经患过水痘,20名患过带状疱疹。903份血清标本中,共检出VZV IgG抗体阳性标本617份,阳性率为68.33%。结论新入伍人员VZV IgG抗体阳性率较低,提示加强水痘疫苗接种,对军队中水痘防控具有重要意义。

经脑脊液宏基因组二代测序确诊的水痘-带状疱疹病毒脑膜脑炎临床分析

目的 探讨水痘-带状疱疹病毒(VZV)脑膜脑炎患者的诊断方法及脑脊液检查特点。方法回顾性分析开封市中心医院收治的15例应用脑脊液二代测序诊断的VZV脑膜脑炎的临床特点及实验室检查结果并行临床分析。结果 15例VZV脑膜脑炎患者中,11例表现为头痛,发热7例,合并皮肤带状疱疹8例,面神经麻痹1例,认知功能障碍4例,癫痫发作2例。脑脊液结果:白细胞数轻-中度升高,以淋巴细胞为主,其中6例氯化物降低,5例乳酸增高。结论 VZV脑膜脑炎患者临床上多表现为头痛,合并发热、皮肤带状疱疹者较多。脑脊液宏基因组二代测序是诊断VZV脑膜脑炎的一种新的有效方法。中枢神经系统VZV主要表现为脑膜炎与脑膜脑炎,抗病毒治疗预后良好。

水痘-带状疱疹病毒特异性细胞免疫及其预测带状疱疹后遗神经痛的价值

目的探讨带状疱疹患者水痘-带状疱疹病毒(Varicella-zoster virus,VZV)特异性细胞免疫的特点,并对发生带状疱疹后遗神经痛(PHN)的预测价值进行分析。方法选择2021年1月至2022年6月于我院体检中心明确为健康的成年人10例作为研究对象,构建VZV特异性组、对照组模型,分析两组间细胞免疫因子之间的差异。选择同时期于我院就诊的带状疱疹(HZ)患者70例作为研究对象,收集初次就诊时患者存在差异的VZV特异性细胞免疫因子指标(后简称指标),而后对患者进行为期半年的随访,对指标预测PHN发生的价值进行分析。结果VZV组患者CD4^(+)T细胞占比低于对照组,而CD8^(+)T细胞及PD-1^(+)CD4^(+)T细胞占比高于对照组,差异有统计学意义(P<0.05)。两组患者PBMC上清液中IFN-γ、IL-2水平比较差异无统计学意义(P>0.05)。VZV组患者PBMC上清液中TNF-α水平高于对照组,差异有统计学意义(P<0.05)。PHN组患者合并前区疼痛占比、多阶段发病占比、发病至开始治疗时间及PBMC上清液的TNF-α水平均高于非PHN组;CD3^(+)T细胞百分比低于非PHN组,差异有统计学意义(P<0.05)。PBMC上清液TNF-α(HR=1.148)是HZ患者PHN发生风险的独立危险因素(P<0.05)。PBMC上清液中TNF-α对于PHN发生具有较好的预测效果(AUC=0.902,P<0.001,95%CI:0.821~0.981)。预测的截断值为>54.36 pg/mL,预测敏感度为82.35%,特异度为85.11%,阳性预测值为66.67%,阴性预测值为93.02%。结论PBMC上清液内TNF-α是影响PHN发生的VZV特异性细胞免疫因子,对于预测HZ患者PHN发生上具有一定的临床意义。

水痘-带状疱疹病毒脑炎/脑膜炎患者预后因素分析

目的分析水痘-带状疱疹病毒再激活导致的脑炎/脑膜炎患者预后因素。方法收集2019年1月至2021年12月39例经脑脊液水痘-带状疱疹病毒(VZV)DNA确诊的VZV脑炎/脑膜炎患者临床资料及出院3个月随访资料,根据是否影响患者的生活质量原则将患者分为预后良好组18例与预后不良组21例,全面分析两组患者一般情况、临床特点以及实验室检查,探讨影响VZV脑炎/脑膜炎预后的因素。结果与预后良好组比较,预后不良组VZV脑炎/脑膜炎患者发热(体温>38℃)比例更高,从出现神经系统症状到开始抗病毒治疗间隔时间明显延长,脑脊液白细胞计数、ADA含量、CRP明显增高,差异均有统计学意义(P<0.05)。多因素Logistic回归分析显示,脑脊液腺苷脱氨酶(ADA)含量(OR=1.279,95%CI=0.996~1.642),从出现神经系统症状到开始抗病毒治疗间隔时间(OR=1.299,95%CI=1.011~1.669)均是患者预后不良的独立危险因素(P<0.05)。结论VZV脑炎/脑膜炎患者出院3个月后出现影响患者生活质量并发症发生率较高。脑脊液ADA含量越高,从出现神经系统症状到开始抗病毒治疗间隔时间越长,患者预后越差。

Severe autoimmune hepatitis triggered by varicella zoster infection

Autoimmune hepatitis (AIH) is a chronic disease of unknown etiology that is characterized by the presence of circulatory autoantibodies and inflammatory histological changes in the liver. Although the pathogenesis of AIH is not known, it is thought that, in a genetically predisposed individual, environmental factors such as viruses can trigger the autoimmune process. Herpes simplex virus, Epstein-Barr virus, measles virus, and hepatitis viruses are thought to play a role in the etiology of AIH. Proteins belonging to these viruses may be similar to the amino acid chains of different autoantigens in the liver, this causes immune cross reactions and liver tissue damage. We report a case of severe AIH following varicella zoster infection in a 23-year-old man, and speculate that, based on the molecular mimicry hypothesis, the liver damage was caused by an immune cross reaction to the viral proteins. Varicella-zoster-induced AIH has not been reported previously.

水痘-带状疱疹病毒引起卡波西水痘样疹一例

卡波西水痘样疹多由单纯疱疹病毒1型引起,水痘-带状疱疹病毒所致较少见。本文报道一例由水痘-带状疱疹病毒引起的卡波西水痘样疹患者,入院初期拟“类天疱疮”治疗下仍有新发水疱,后结合组织病理、病原宏基因组学检测示水痘-带状疱疹病毒阳性,最终诊断为卡波西水痘样疹,给予抗病毒治疗后好转。