Clinical characteristics and treatment of severe encephalitis associated with neurogenic pulmonary edema caused by enterovirus 71 in China

BACKGROUND： Hand-foot-mouth disease has become a major public health issue in children in China. In the present prospective study we investigated the clinical characteristics and emergency management of children with severe encephalitis associated with NPE caused by enterovirus 71.METHODS： The study was conducted in 2 pediatric intensive care units （PICUs） over a 2-month period. Clinical records were reviewed of critically ill children with severe encephalitis associated with NPE caused by EV71 who were admitted to PICUs during the period of May to June 2008 in Fuyang.RESULTS： We reviewed the complete records of 36 children, of whom 23 （63.9%） were male and 13 （36.1%） female. Their age ranged from 4 to 48 months, with an average of 15.8 months. All children except one were under 3 years of age. The overall mortality in these children was 19.4%. The average duration of critical life threatening signs and symptoms was 2.1 days （12 hours-5 days）. Nervous system diseases included brainstem encephalitis in 27 children （75%）, brainstem encephalitis associated with myelitis in 6 children （16.7%）, and general encephalitis in 3 chidren （8.3%）, respectively. In 12 patients of NPE （33.3%） pink or bloody bubble sputum and asymmetric pulmonary edema or hemorrhage was the primary manifestation but no typical exanthema was observed. Five children died of acute onset of NPE and / or pulmonary hemorrhage with rapid progression of cardiopulmonary failure within hours after admission. Therapeutic management consisted of mechanical ventilation and administration of mannitol, methylprednisolone, intravenous immunoglobulin （IVIG） and vasoactive drugs, associated with the need of fluid volume resuscitation in 9 （25%） of the 36 children.CONCLUSION： In children less than 3 years of age found to be affected by severe EV71 encephalitis associated with NPE, one fifth may die. The major organ systems infected by severe EV71 include the central nervous system, the respiratory system, and the cardiovascular system. Early diagnosis and evaluation, respiratory support, treatment of intracranial hypertension, and mainttenance of function of the cardiovascular system are the most important therapeutic measures.

Therapeutic and prevention strategies against human enterovirus 71 infection

Human enterovirus 71(HEV71) is the cause of hand,foot and mouth disease and associated neurological complications in children under five years of age.There has been an increase in HEV71 epidemic activity throughout the Asia-Pacific region in the past decade,and it is predicted to replace poliovirus as the extant neurotropic enterovirus of highest global public health significance. To date there is no effective antiviral treatment and no vaccine is available to prevent HEV71 infection. The increase in prevalence, virulence and geographic spread of HEV71 infection over the past decade provides increasing incentive for the development of new therapeutic and prevention strategies against this emerging viral infection. The current review focuses on the potential, advantages and disadvantages of these strategies. Since the explosion of outbreaks leading to large epidemics in China, research in natural therapeutic products has identified several groups of compounds with anti-HEV71 activities. Concurrently, the search for effective synthetic antivirals has produced promising results. Other therapeutic strategies including immunotherapy and the use of oligonucleotides have also been explored. A sound prevention strategy is crucial in order to control the spread of HEV71. To this end the ultimate goal is the rapid development, regulatory approval and widespread implementation of a safe and effective vaccine. The various forms of HEV71 vaccine designs are highlighted in this review. Given the rapid progress of research in this area, eradication of the virus is likely to be achieved.

Comparative Genomic Analysis of Enterovirus 71 Revealed Six New Potential Neurovirulence-associated Sites

In the present study,the complete genomes of four common（4/EV71/Wenzhou/CHN/2014,15/EV71/Wenzhou/CHN/2014,116/EV71/Wenzhou/CHN/2014,and 120/EV71/Wenzhou/CHN/2014）and two virulent（11/EV71/Wenzhou/CHN/2014and 109/EV71/Wenzhou/CHN/2014）enterovirus 71（EV71）isolates were sequenced and described.They are 7405 bp in length and belong to EV71 sub-genotype C4 （C4a cluster）.

Evaluation of Reverse Transcription Loop-Mediated Isothermal Amplification assays for Rapid Detection of Human Enterovirus 71 and Coxsackievirus A16 in Clinical Samples

A sensitive reverse transcription loop-mediated isothermal amplification (RT-LAMP) assay for human enterovirus 71 (EV71) and Coxsackievirus A16 (CVA16) infection was further evaluated. The one step reaction was performed in a single tube at 65?C for 45 min for EV71 and 35 min for CVA16. The detection limits of RT-LAMP assays for both EV71 and CVA16 were 0.1 of a 50% tissue culture infective dose (TCID50) per reaction, based on 10—Fold dilutions of a titrated EV71 or CVA16 strain. The specific assay showed there were no cross-reactions with Coxsackievirus A (CVA) viruses (CVA 2, 4, 5, 7, 9, 10, 14, and 25), Coxsackievirus B (CVB) viruses (CVB 1, 2, 3, 4, and 5) or ECHO viruses (ECHO 3, 6, 11, and 19). In parallel with commercial quantitative real-time polymerase chain reaction (qRT-PCR) diagnostic kits for EV71 and CVA16, the RT-LAMP assay was evaluated with 515 clinical specimens, the results showed the RT-LAMP assay and the qRT-PCR assay were in complete agreement for 513/515 (99.6%) of the specimens. Two samples with discrepant results from two methods were further verified by nested reverse transcription polymerase chain reaction (nRT-PCR) assay and sequencing to be true positives for CVA16. In conclusion, RT-LAMP assay is demonstrated to be a sensitive and specific assay and have a great potential for the rapid and visual screening of EV71 and CVA16 in China, especially in those resource-limited hospitals and rural clinics of provincial and municipal regions.

灰树花水溶物对EV71病毒的抑制作用

【目的】探讨灰树花水溶物(GFWE)的化学成分及其对EV71病毒的抑制作用,为促进灰树花综合利用、提高其经济附加值,以及开发预防和治疗EV71病毒感染的功能性食品提供依据。【方法】采用色谱法测定了GFWE的主要化学成分组成、多糖组成和分子质量。基于体外细胞培养采用CCK-8法确定了GFWE的安全上样量;以EV71病毒感染Vero细胞为模型,探究GFWE对EV71病毒的抑制率及对Vero细胞形态的影响,并采用荧光定量PCR检测了EV71病毒衣壳蛋白(VP1)编码基因mRNA的表达水平,初步评价了GFWE对EV71病毒的抑制作用。【结果】GFWE主要由低分子质量多糖、氨基酸、肽及其衍生物组成。GFWE富含的13种氨基酸中包含7种必需氨基酸;其多糖由葡萄糖、半乳糖、盐酸氨基葡萄糖和古罗糖醛酸4种单糖组成,物质的量比为0.907∶0.038∶0.029∶0.026,重均分子质量分别为15.67、10.10、6.60 ku和<1.00 ku。GFWE表现出较高的抗EV71病毒活性,100、200μg·mL^(-1) GFWE对EV71病毒的抑制率分别为91.32%、91.83%,25~400μg·mL^(-1) GFWE能显著降低EV71 VP1 mRNA的表达水平。【结论】GFWE主要由低分子质量多糖、氨基酸、肽及其衍生物组成,具有较高的抗EV71病毒活性,能够抑制感染EV71病毒的Vero细胞中VP1的合成。

血清25-羟基维生素D与EV71感染手足口病患儿Th1/Th2细胞因子及病情进展关系研究

目的血清25-羟基维生素D[25-(OH)D]与肠道病毒71型(EV71)感染手足口病患儿辅助性T(Th)1/Th2细胞因子及病情进展的关系研究。方法选择2020年10月至2023年10月在我院就诊的135例EV71感染手足口病患儿作为研究对象,依据病情严重程度分为普通型组(n=95)、重型组(n=40),对比两组血清25-(OH)D、Th1/Th2细胞因子[血清白细胞介素-2(IL-2)、肿瘤坏死因子-α(TNF-α)、血清IL-6]水平,Pearson相关性分析血清25-(OH)D、Th1/Th2细胞因子的关系,多因素Logistic回归模型探讨血清25-(OH)D与病情进展的关系。结果两组血清25-(OH)D水平比较,重型组更低,血清IL-2、TNF-α、IL-6水平比较,重型组更高(P<0.05);血清25-(OH)D与IL-2/TNF-α/IL-6水平负相关(r=-0.344、-0.344、-0.424,P均<0.05);重型组血清25-(OH)D、体液免疫IgG水平及个人卫生习惯良好比例低于普通型组,手足口病病史与白细胞(中性粒细胞)计数升高比例高于普通型组(P<0.05);血清25-(OH)D为患儿病情进展的保护因素(P<0.05),手足口病史、CRP升高为患儿病情进展独立危险因素(P<0.05)。结论血清25-(OH)D与EV71感染手足口病患儿IL-2、TNF-α、IL-6水平均呈负相关,且血清25-(OH)D是EV71感染手足口病患儿病情进展的保护因素,应重视对患儿血清25-(OH)D水平的动态追踪并合理补充维生素D。

T淋巴细胞亚群、炎症因子在感染EV71的手足口病患儿病情评估中的应用

目的研究T淋巴细胞亚群、炎症因子在感染EV71的手足口病患儿病情评估中的应用。方法选取2022年3月至2023年3月我院收治的78例感染EV71的手足口病患儿为研究对象,根据潜伏期患儿疾病严重程度分为观察组(重症病例)和对照组(普通病例)各39例。两组均检测T淋巴细胞亚群、血清炎症因子水平,绘制受试者工作曲线(ROC)分析评估效能。结果观察组患儿的炎症因子水平高于对照组,CD3^(+)、CD4^(+)水平更低于对照组,CD4^(+)/CD8^(+)水平高于对照组(P<0.05);ROC结果显示:感染EV71的手足口病患儿IL-1、IL-6、TNF-α、CD3^(+)、CD4^(+)、CD4^(+)/CD8^(+)均存在病情评估价值(P<0.05,AUC>0.5)。结论不同病情感染EV71的手足口病患儿T淋巴细胞亚群及炎症因子存在差异,检测上述指标有助于临床病情评估。

Gp78 regulates PMP22 and causes ER stress and autophagy in EV71-VP1-overexpressing mouse Schwann cells

Background:During Enterovirus type 71(EV71)infection,the structural viral protein 1(VP1)activates endoplasmic reticulum(ER)stress associated with peripheral myelin protein 22(PMP22)accumulation and induces autophagy.However,the specific mechanism behind this process remains elusive.Methods:In this research,we used the VP1-overexpressing mouse Schwann cells(SCs)models co-transfected with a PMP22 silencing or Autocrine motility factor receptor(AMFR/gp78)overexpressing vector to explore the regulation of gp78 on PMP22 and its relationship with autophagy and apoptosis.Results:The activity of gp78 could be influenced by EV71-VP1,leading to a decrease in the ubiquitination and degradation of PMP22,resulting in PMP22 accumulation in ER.In VP1-overexpressing mouse SCs,all three ER stress sensors,including pancreatic endoplasmic reticulum kinase(PERK),activating transcription factor 6(ATF6)and inositol-requiring enzyme 1(IRE1)and the related downstream signals(C/EBP-homologous protein(CHOP)and Caspase 12)were activated,as well as the ER-resident chaperone Glucose-regulated protein 78(GRP78).In addition,VP1 upregulated the autophagy marker Microtubule-associated protein 1 light chain 3 beta(LC3B),while PMP22 silencing or gp78 overexpression reversed the phenomenon.Meanwhile,PMP22 silencing or gp78 overexpression increased proliferation of EV71-VP1-transfected mouse SCs.Conclusion:Gp78 could regulate PMP22 accumulation through ubiquitination degradation and cause ER stress and autophagy in EV71-VP1-overexpressing mouse SCs.Therefore,the gp78/PMP22/ER stress axis might emerge as a promising therapeutic target for myelin and neuronal damage induced by EV71 infection.

学龄前儿童接种肠道病毒71型(EV71)疫苗状况及家长对其接种意愿影响因素

目的:分析学龄前儿童接种肠道病毒71型(EV71)疫苗状况及家长对其接种意愿影响因素。方法:研究选取本区2022年1月至2023年12月行健康体检学龄前儿童300例为研究对象,采集其疫苗接种状况,采用单因素及Logistic回归分析家长对学龄前儿童接种意愿影响因素。结果:300例学龄前儿童中,接种EV71型疫苗儿童71例,接种率23.67%。学龄前儿童EV71型疫苗接种情况单因素分析结果显示,学龄前儿童EV71型疫苗接种情况与性别、年龄、少儿医保、足月分娩、出生体质量、儿童来源以及是否顺产等因素无统计学意义(P>0.05);学龄前儿童家长对EV71型疫苗接种意愿单因素分析结果显示,学龄前接种EV71型疫苗儿童与未接种疫苗儿童的家长对手足口病认知程度、对EV71型疫苗了解程度、家长学历、家庭月收入等差异有统计学意义(P<0.05);Logistic回归分析显示,家长对手足口病认知程度、对EV71型疫苗了解程度、家长学历、家庭月收入是影响其接种意愿的独立影响因素(P<0.05)。结论:学龄前儿童EV71疫苗接种率相对较低,家长对手足口病及EV71疫苗的了解程度、家长学历以及家庭月收入等是影响家长对学龄前儿童接种EV71疫苗意愿的独立影响因素。

CD25基因多态性与EV71感染手足口病患儿易感性及严重性的关系

目的:探讨CD25基因多态性与肠道病毒71型(EV71)感染手足口病(HFMD)患儿易感性及严重性的关系。方法:将2020年11月—2022年11月我院收治的122例EV71感染HFMD患儿作为本次研究对象(HFMD组),根据疾病严重程度分为轻症组(n=79)和重症组(n=43)2个亚组。另外将同时期在我院进行健康检查的150例健康儿童纳入对照组。采用限制性片段长度多态性聚合酶链反应(PCR-RFLP)技术鉴定CD25基因rs7072793位点基因分型;采用Hardy-Weinberg遗传平衡度检验对样本代表性进行评估;采用多因素Logistic回归分析探讨EV71感染重症HFMD发病的危险因素。结果:对照组和HFMD组CD25基因rs7072793位点基因型符合Hardy-Weinberg遗传平衡定律,样本具有代表性(P>0.05)。对照组CD25基因rs7072793位点CC、CT、TT基因型频率和C、T等位基因频率与HFMD组比较,差异有统计学意义(P<0.05)。轻症组CD25基因rs7072793位点CC、CT、TT基因型频率和C、T等位基因频率与重症组比较,差异有统计学意义(P<0.05)。多因素Logistic回归分析结果显示,脑电图结果异常、CD25基因rs7072793位点TT基因型、CD25基因rs7072793位点T等位基因是EV71感染重症HFMD发病的独立危险因素(P<0.05)。结论:CD25基因rs7072793位点多态性与EV71感染HFMD患儿的易感风险和病情严重程度存在关联,且携带TT基因型、T等位基因患儿进展为重症的风险更高。

Genetic Analysis of the VP1 Region of Human Enterovirus 71 Strains Isolated in Fuyang,China,During 2008

Enterovirus 71 （EV71） is a common cause of Hand, foot, and mouth disease （HFMD） and may also cause severe neurological diseases, such as encephalitis and poliomyelitis-like paralysis. To examine the genetic diversity of EV71, we determined and analyzed the complete VP1 sequences （891 nueleotides） from nine EV71 strains isolated in Fuyang, China. We found that nine EV71 strains isolated were over 98% homologous at the nucleotide level and 93%-100% homologous tO members of the C4 subgenogroup. At the amino acid level, these Fuyang strains were 99% -100% homologous to one another, 97%-100% homologous to members of the C4 subgenogroup, and the histidine（H） at amino acid position 22 was conserved among the Fuyang strains. The results indicate that Fuyang isolates belong to genotype C4, and an H at position 22 appears to be a marker for the Fuyang strains.

HPLC-UV法检测EV71-CA16二价手足口病灭活疫苗原液相关抗原纯度的方法建立与评价

为建立一种准确可靠的高效液相色谱-紫外(HPLC-UV)方法,检测EV71-CA16二价手足口病(HFMD)灭活疫苗原液中的相关抗原,肠道病毒71型(EV71)和柯萨奇病毒A组16型(CA16)的纯度。本文采用Waters体积排阻色谱柱(SEC,UltrahydrogelTM 2507.8×300 mm,6μm),流动相为0.01 mol/L的PBS中再加入0.1 mol/L氯化钠溶液,等度洗脱,流速0.3 mL/min,检测波长280 nm,进样量50μL,柱温21℃,进行EV71与CA16病毒原液的纯度检测,并对该方法的检测限、拖尾因子、专属性、重复性及检测范围进行验证。结果显示,2种抗原的灵敏度溶液的信噪比(S/N)分别为37.053和47.710,均远大于3,各试样的拖尾因子均小于3;CA16原液和EV71原液经HPLC分离纯化后的目标抗原峰馏分经SDS-PAGE和Western-Blot特异性鉴定,结果显示,色谱峰样品组成分别为CA16和EV71的2种病毒衣壳的结构蛋白,表明本检测方法专属性高。不同浓度的EV71与CA16病毒抗原经多次检测后,各浓度条件下的峰面积百分比与保留时间的RSD均小于1%,重复性良好。不同抗原浓度批样品检测结果显示,CA16原液抗原浓度在89 U/mL~26398 U/mL之间,EV71原液抗原浓度在170 U/mL~9074 U/mL之间时,2种抗原溶液经多次检测统计显示峰面积百分比与保留时间的RSD均小于1%,本方法在该抗原浓度范围内准确可靠,适用于EV71-CA16二价手足口病灭活疫苗原液中病毒抗原纯度的检测。

Antiviral Activity of GuiQi Polysaccharides against Enterovirus 71 in vitro

In this study,we have investigated the antiviral activity of GuiQi polysaccharides (GQP) upon enterovirus 71 (EV71) in vitro.An assay using methyl thiazolyl tetrazolium (MTT),and analyses of cytopathic effects (CPE)were used to examine the antiviral activity of GQP upon Vero cells infected with EV71.The results revealed that GQP at concentrations below 31.2μg/mL exhibited significant antiviral effects upon EV71 when applied under three different experimental protocols.GQP was most strongly active in preventing the adsorption of EV71 to target cells and in this respect it was significantly more effective than ribavirin.In addition,it was clear that GQP could inhibit viral replication when added to cells 2 h after infection,but if added at the point of infection its effect was weak.GQP is considered to be less toxic than ribavirin,and may warrant further evaluation as a possible agent in the treatment of hand,foot and mouth disease (HFMD).

Expression,purification and characterization of enterovirus-71 virus-like particles

AIM： Enterovirus 71 （EV71） has been implicated as the etiological agent responsible for the recent outbreaks of hand, foot and mouth disease associated with severe neurological diseases in the Asia-Pacific region. METHODS： The assembly process was hypothesized to occur via an orchestrated proteolytic processing of the P1 precursor by the viral protease 3CD. To test this hypothesis, we constructed 3 recombinant baculoviruses： Bac-P1 expressing P1; Bac-3CD expressing 3CD; and Bac-P1-3CD co-expressing P1 and 3CD. RESULTS： Both single infection by Bac-P1-3CD and coinfection by Bac-P1 and Bac-3CD resulted in correct cleavage of P1 to yield individual proteins VP0, VP1 and VP3, while the former approach yielded higher VLP production. In the cells, the structural proteins selfassembled into clusters of virus-like particles （VLP） resembling the authentic EV71 particle aggregates. After ultracentrifugation purification, the dispersed VLPs were indistinguishable from the authentic virus in size, appearance, composition and surface epitopes, as determined by SDS-PAGE, Western blot, transmission electron microscopy and immunogold labeling. CONCLUSION： Our data, for the first time, suggest that in insect cells EV71 structural proteins adopt a processing and assembly pathway similar to poliovirus assembly. The preservation of particle morphology and composition suggest that the VLP may be a valuable vaccine candidate to prevent EV71 epidemics.

Hand Foot and Mouth Disease Due to Enterovirus 71 in Malaysia

Hand foot and mouth disease is a febrile sickness complex characterized by cutaneous eruption (exanthem) on the palms and soles with simultaneous occurrence of muco-cutanous vesiculo-ulcerative lesions (enanthem) affecting the mouth. The illness is caused by a number of enteroviruses with coxsackievirus A16 and enterovirus 71 as the main causative agents. Human enterovirus 71 (EV71) belongs to the species Human enterovirus A under the genus Enterovirus within the family Picornaviridae. EV71 has been associated with an array of clinical diseases including hand foot and mouth disease (HFMD), aseptic meningitis, encephalitis and poliomyelitis-like acute flaccid paralysis. A large outbreak of HFMD due to highly neurovirulent EV71 emerged in Malaysia in 1997, and caused 41 deaths amongst young children. In late 2000, a recurrence of an outbreak of HFMD occurred in Malaysia with 8 fatalities in peninsular Malaysia. Outbreak of HFMD due to EV71 recurred in 2003 with an unknown number of cases and mortalities. A similar outbreak of HFMD with 2 recorded deaths in young children occurred in peninsular Malaysia in late 2005 and this was followed by a larger outbreak in Sarawak (Malaysian Borneo) with 6 reported fatalities in the early part of 2006. The current on-going outbreak of HFMD started in peninsular Malaysia in epidemiological week 12 of 2010. As with other HFMD outbreaks in Malaysia, both EV71 and CA16 were the main aetiological viruses isolated. In similarity with the HFMD outbreak in 2005, the isolation of CA16 preceded the appearance of EV71. Based on the VP1 gene nucleotide sequences, 4 sub-genogroups of EV71 (C1, C2, B3 and B4) co-circulated and caused the outbreak of hand, foot and mouth disease in peninsular Malaysia in 1997. Two sub-genogroups (C1 and B4) were noted to cause the outbreak in 2000 in both peninsular Malaysia and Sarawak. EV71 of sub-genogroup B5 with smaller contribution from sub-genogroup C1 caused the outbreak in 2003. In the 2005 outbreak, besides the EV71 strains of sub-genogroup C1, EV71 strains belonging to sub-genogroup B5 were isolated but formed a cluster which was distinct from the EV71 strains from the sub-genogroup B5 isolated in 2003. The four EV71 strains isolated from clinical specimens of patients with hand, foot and mouth disease in the Sarawak outbreak in early 2006 also belonged to sub-genogroup B5. Phylogenetic analysis of the VP1 gene suggests that the EV71 strains causing the outbreak in Sarawak could have originated from peninsular Malaysia. Epidemiological and molecular data since 1997 show the recurrence of HFMD due to EV71 in Malaysia every 2 to 4 years. In each of the past outbreaks, more than one sub-genogroup of the virus co-circulate.

梧州市城区5岁以下儿童家长手足口病认知与EV71疫苗接种意愿调查研究

调查研究梧州市城区5岁以下儿童家长对手足口病的认知水平与EV71疫苗接种意愿。方法 调查研究起于2021.05,止于2022.05,通过整群随机抽样从梧州市城区12家社区卫生服务中心抽取8家,对卫生服务中心接种门诊日当天带领儿童前来接受预防接种的5岁及以下儿童家长进行面访,填写调查问卷。本次共调研对象1663人。调查内容为儿童家长手足口病认知情况,并分析影响其疫苗接种意愿的影响因素。结果 梧州市城区5岁以下儿童家长对手足口病的认知水平一般,有待接受健康教育,提升相关知识知晓率。有近84%的家长愿意带领孩子接种EV71型疫苗,表示多数家长的预防意识较强。结论 手足口病是危害幼儿的主要传染疾病之一,为保障孩子健康生长和发育,家长应当积极了解疾病相关知识,提高认知水平,并通过多种渠道了解疾病及其预防措施,主动带领幼儿接种EV71疫苗,能够实现良好的预防效果。

Human IgG Fc promotes expression, secretion and immunogenicity of enterovirus 71 VP1 protein

Enterovirus （EV71） can cause severe neurological diseases, but the underlying pathogenesis remains unclear. The capsid protein, viral protein 1 （VP1）, plays a critical role in the pathogenicity of EVT1. High level expression and secretion ofVP 1 protein are necessary for structure, function and immunogenicity in its natural conformation. In our previous studies, 5 codon-optimized VP 1 DNA vaccines, including wt-VP 1, tPA-VP 1, VP l-d, VP 1-hFc and VP 1 - mFc, were constructed and analyzed. They expressed VP1 protein, but the levels of secretion and immunogenicity of these VP1 constructs were significantly different （P〈0.05）. In this study, we further investigated the protein lev- els of these constructs and determined that all of these constructs expressed VP1 protein. The secretion level was increased by including a tPA leader sequence, which was further increased by fusing human IgG Fc （hFc） to VP1. VP 1-hFc demonstrated the most potent immunogenicity in mice. Furthermore, hFc domain could be used to purify VPI-hFc protein for additional studies.

直肠滴入中药对CoxA16、EV71肠道病毒感染手足口病的疗效

目的观察直肠滴入中药对CoxA16、EV71肠道病毒感染手足口病的疗效。方法选取2019年8月—2022年8月贵州水矿控股集团有限公司总医院CoxA16、EV71肠道病毒感染手足口病患儿85例,按照随机数表法分为观察组(42例)和对照组(43例),其中对照组患儿给予利巴韦林治疗,观察组患儿给予直肠滴入中药治疗。对比两组患儿治疗前后口腔疱疹、发热、皮疹等症状的评分,治疗前后患儿炎症因子、免疫指标水平及两组患儿治疗后不良反应发生率。结果治疗前,两组患儿的口腔疱疹、发热、皮疹评分差异无统计学意义(P>0.05),治疗后,两组患儿的口腔疱疹、发热、皮疹评分均降低,并且治疗后观察组患儿的以上症状评分低于对照组(P<0.05);治疗后,两组患儿白细胞介素(IL)-6、IL-8、肿瘤坏死因子(TNF)-α均降低,并且治疗后观察组患儿的以上降低幅度大于对照组(P<0.05);治疗后,两组患儿CD4^(+)、CD3^(+)、CD4^(+)/CD8^(+)水平均升高,CD8^(+)水平降低,并且治疗后观察组患儿的变化幅度大于对照组(P<0.05);观察组患儿不良反应发生率为4.76%,对照组患儿不良反应发生率为18.60%,观察组不良反应发生率低于对照组(P<0.05)。结论给予CoxA16、EV71肠道病毒感染手足口病患儿直肠滴入中药治疗,能减轻患儿临床症状及炎性反应,改善免疫功能,且不良反应少,值得借鉴。

Positive Selection Analysis of VP1 Genes of Worldwide Human Enterovirus 71 Viruses

Human enterovirus 71 viruses have been long circulating throughout the world. In this study, we performed a positive selection analysis of the VP1 genes of capsid proteins from Enterovirus 71 viruses. Our results showed that although most sites were under negative or neutral evolution, four positions of the VP1 genes were under positive selection pressure. This might account for the spread and frequent outbreaks of the viruses and the enhanced neurovirulence. In particular, position 98 might be involved in neutralizing antibodies, modulating the virus-receptor interaction and enhancing the virulence of the viruses. Moreover, both positions 145 and 241 might correlate to determine the receptor specificity. However, these positions did not display much difference in amino acid polymorphism. In addition, no position in the VP1 genes of viruses isolated from China was under positive selection.

铝吸附EV71-CA16二价手足口病灭活疫苗CA16抗原解离方法研究

为建立铝吸附EV71-CA16二价手足口病灭活疫苗CA16抗原解吸附的方法,用于CA16抗原含量的检测。本文采用单一变量的方法,分别固定柠檬酸钠、10%曲拉通与20%二乙醇胺的比例以确定最佳解离液配方,在此基础上通过不同孵育温度和时间处理疫苗成品,ELISA法检测解离后的CA16抗原含量,计算抗原回收率,确定最佳解离液配方及解离条件,并考察其重复性。结果显示,解离液最佳方法为20%二乙醇胺1.25 mL、10%曲拉通50μL、柠檬酸钠浓度为14%,由0.01M PBS定容至10 mL,室温(18~25℃)孵育0.5 h解离疫苗成品,经解离后的CA16的抗原含量达1800 U/mL,回收率在90%以上,线性相关系数R2值大于0.97,重复试验的变异系数均小于5%。结果表明,该解离方法回收率高,重复性好,检测结果准确。