HERPES

疱疹
  • 文章类型: Journal Article
    胶质瘤,包括近80%的脑恶性肿瘤,胶质母细胞瘤是最具侵袭性的亚型,这是一个巨大的挑战。尽管多学科护理,包括手术和放化疗,预后依然严峻,强调创新治疗策略的必要性。血脑屏障使药物进入复杂化,多样的组织病理学阻碍了靶向治疗。溶瘤疱疹病毒(oHSV),特别是HSV1716、G207和rQNestin34.5v,通过在肿瘤细胞中选择性复制,在神经胶质瘤治疗中显示出希望。临床前和临床研究证明了oHSV的安全性和有效性,T-Vec被FDA批准.然而,挑战,如病毒递送限制和抗病毒反应持续存在。OHSV和环磷酰胺(CPA)的组合解决了这些挑战,证明转基因表达和病毒活性增加。CPA的免疫抑制特性,特别是在节制时间表中,增强oHSV功效,支持这种联合治疗复发性恶性神经胶质瘤的发展。具有oHSV的CPA增强病毒溶瘤作用并延长存活。CPA的免疫调节作用,抑制调节性T细胞,提高OHSV效率。虽然障碍依然存在,这种协同方法为改善结果提供了希望,需要进一步的研究和临床验证。
    Gliomas, comprising nearly 80% of brain malignancies, present a formidable challenge with glioblastomas being the most aggressive subtype. Despite multidisciplinary care, including surgery and chemoradiotherapy, the prognosis remains grim, emphasizing the need for innovative treatment strategies. The blood-brain barrier complicates drug access, and the diverse histopathology hinders targeted therapies. Oncolytic herpes viruses (oHSVs), particularly HSV1716, G207, and rQNestin34.5v, show promise in glioma treatment by selectively replicating in tumor cells. Preclinical and clinical studies demonstrate the safety and efficacy of oHSVs, with T-Vec being FDA-approved. However, challenges like viral delivery limitations and antiviral responses persist. The combination of oHSVs and combining cyclophosphamide (CPA) addresses these challenges, demonstrating increased transgene expression and viral activity. The immunosuppressive properties of CPA, particularly in metronomic schedules, enhance oHSV efficacy, supporting the development of this combination for recurrent malignant gliomas. CPA with oHSVs enhances viral oncolysis and extends survival. CPA\'s immunomodulatory effects, suppressing regulatory T cells, improve oHSV efficiency. While obstacles remain, this synergistic approach offers hope for improved outcomes, necessitating further research and clinical validation.
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  • 文章类型: Journal Article
    许多疱疹病毒相关疾病的预防和治疗是基于抗病毒治疗的利用,然而,耐药性的发展限制了治疗的成功。目前不存在单一数据库编目抗性突变,这阻碍了序列数据用于患者管理。因此,我们开发了HerpesDRG,一个耐药突变数据库,包含所有已知的耐药基因和当前的治疗选择,从可用基因型到表型文献的系统综述。该数据库与R包一起发布,该R包提供了一种简单的方法来从常见的sanger和下一代测序数据中进行抗性变体注释和临床意义分析。这是人类疱疹病毒(HHV)耐药性突变的第一个公开可用和社区可维护的数据库,为解决HHV耐药性的研究人员和临床医生社区开发。
    The prevention and treatment of many herpesvirus associated diseases is based on the utilization of antiviral therapies, however therapeutic success is limited by the development of drug resistance. Currently no single database cataloguing resistance mutations exists, which hampers the use of sequence data for patient management. We therefore developed HerpesDRG, a drug resistance mutation database that incorporates all the known resistance genes and current treatment options, built from a systematic review of available genotype to phenotype literature. The database is released along with an R package that provides a simple approach to resistance variant annotation and clinical implication analysis from common sanger and next generation sequencing data. This represents the first openly available and community maintainable database of drug resistance mutations for the human herpesviruses (HHV), developed for the community of researchers and clinicians tackling HHV drug resistance.
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  • 文章类型: Journal Article
    自身免疫性多内分泌病-念珠菌病-外胚层营养不良(APECED)是一种先天性免疫错误,影响多种内分泌器官和念珠菌病的易感性。每个都有自身免疫基础。最近,高滴度中和性抗I型干扰素(IFN)自身抗体与APECED患者中SARS-CoV-2和水痘带状疱疹病毒感染的严重程度增加有关.检查对巨细胞病毒(CMV)的免疫力,我们发现APECED患者(N=19)的抗CMVIgG抗体患病率高于44名健康对照(90%vs64%,p=0.04);它们的IgG水平相似的差异没有达到显著性(95±74vs64±35IU/mL,.).相比之下,CMV特异性T细胞的频率较低(804±718/百万对1591±972/百万PBMCp=0.03)。我们在APECED患者或单独的胸腺瘤患者队列中发现抗CMVIgG和抗IFN抗体水平之间没有相关性(n=70),超过60%的人也有抗IFN抗体。我们的结果表明,APECED患者对CMV的反应失调,并强调了病毒感染的免疫缺陷是疾病谱的一部分。
    Autoimmune polyendocrinopathy-candidiasis-ectodermal dystrophy (APECED) is an inborn error of immunity affecting both multiple endocrine organs and susceptibility to candidiasis, each with an autoimmune basis. Recently, high titer neutralizing anti-type I interferon (IFN) autoantibodies have been linked with increased severity of SARS-CoV-2 and varicella zoster virus infections in APECED patients. Examining immunity against cytomegalovirus (CMV), we found a higher prevalence of anti-CMV IgG antibodies in patients with APECED (N = 19) than in 44 healthy controls (90% vs 64%, p = 0.04); the similar difference in their IgG levels did not achieve significance (95 ± 74 vs 64 ± 35 IU/mL, ns.). In contrast, the frequency of CMV-specific T cells was lower (804 ± 718/million vs 1591 ± 972/million PBMC p = 0.03). We saw no correlations between levels of anti-CMV IgG and anti-IFN antibodies in APECED patients or in a separate cohort of patients with thymoma (n = 70), over 60% of whom also had anti-IFN antibodies. Our results suggest a dysregulated response to CMV in APECED patients and highlight immunodeficiency to viral infections as part of the disease spectrum.
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  • 文章类型: Journal Article
    背景:脑炎的早期诊断涉及识别神经炎症的体征,包括脑脊液(CSF)细胞增多症。然而,已经描述了脑炎中没有CSF细胞增多,最明显的是自身免疫性脑炎。我们检查了与不存在或存在CSF白细胞胞吞作用(≥5个细胞/μL)相关的临床特征和结果,及时诊断和治疗脑炎。
    方法:这项回顾性研究比较了597例全因脑炎成年患者的初始CSF分布。
    结果:在597名患者中,446(74.7%)有CSF胞质增多,而151(25.3%)没有。脑脊液细胞增多更常见于感染病例(200/446,44.8%),连同59例(13.2%)自身免疫性病例,主要包括抗NMDAR脑炎(37/59,62.7%)。值得注意的是,无细胞增多症的组感染性脑炎(47/151,31.1%)和自身免疫性脑炎(38/151,25.92%;p>0.05)的比例相似.在那些患有传染性脑炎的人中,47/247(19%)无细胞增多症,包括18/76(23.7%)的HSV-1脑炎。细胞增多症的缺乏与阿昔洛韦的给药速率降低相关(无细胞增多症患者为47.7%71.1%的细胞增多症患者,p<0.001)。尽管白细胞增多与入院时的一些临床严重程度指标相关,例如完全不反应性(FOUR)评分≤14,但与死亡率或住院时间无关。
    结论:脑脊液细胞增多是诊断脑炎的重要标准,但是25.3%的全因脑炎患者和23.7%的HSV-1脑炎患者在最初的LP中没有细胞增多。在疑似脑炎的患者中,在没有细胞增多的情况下,不应延迟阿昔洛韦的开始。
    BACKGROUND: Early diagnosis of encephalitis involves identifying signs of neuroinflammation, including cerebrospinal fluid (CSF) pleocytosis. However, absence of CSF pleocytosis in encephalitis has been described, most notably in autoimmune encephalitis. We examined clinical characteristics and outcomes associated with the absence or presence of CSF white blood cell pleocytosis (≥ 5 cells/µL), to inform timely diagnosis and management of encephalitis.
    METHODS: This retrospective study compares initial CSF profiles in 597 adult patients with all-cause encephalitis.
    RESULTS: Of the 597 patients, 446 (74.7%) had CSF pleocytosis while 151 (25.3%) did not. CSF pleocytosis occurred more commonly in infectious cases (200/446, 44.8%), along with 59 (13.2%) autoimmune cases, comprised chiefly of anti-NMDAR encephalitis (37/59, 62.7%). Notably, the group without pleocytosis was comprised of similar proportions of infectious (47/151, 31.1%) and autoimmune (38/151, 25.92%; p>0.05) encephalitis. Among those with infectious encephalitis, 47/247 (19%) had absent pleocytosis, including 18/76 (23.7%) with HSV-1 encephalitis. The absence of pleocytosis was associated with a decreased rate of acyclovir administration (47.7% in patients without pleocytosis vs. 71.1% in patients with pleocytosis, p<0.001). Despite pleocytosis being associated with some measures of clinical severity at admission such as a Full Outline of UnResponsiveness (FOUR) score ≤14, it was not associated with mortality or prolonged hospitalization.
    CONCLUSIONS: CSF pleocytosis is an important criterion for encephalitis diagnosis, but 25.3% of patients with all-cause encephalitis and 23.7% of those with HSV-1 encephalitis exhibit absence of pleocytosis on initial LP. Acyclovir initiation should not be delayed in the absence of pleocytosis in patients with suspected encephalitis.
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  • 文章类型: Journal Article
    随着世界从COVID-19大流行中恢复过来,MPXV案件的死灰复燃引起了严重关注。MPXV与流感和感冒等常见疾病的早期临床相似性,再加上其进展性皮疹与其他感染的相似之处,强调及时准确诊断的重要性。在感染中,天花在临床上最接近MPXV,梅毒和水痘带状疱疹中也出现类似MPXV阶段的皮疹。对MPXV的全面审查,疱疹,梅毒发生了,包括结构和形态特征,起源,传输模式,和计算研究。PubMed在MPXV上的文献检索,使用MeSH关键术语,产生了1904年的结果,分析揭示了与性传播疾病的突出联系。更深入地探索MPXV,单纯疱疹病毒(HSV),和梅毒进一步揭示了疾病的相互联系和地理相关性。这些发现强调需要全面了解这些相互关联的传染因子,以更好地控制和管理。
    As the world recovers from the COVID-19 pandemic, a resurgence in MPXV cases is causing serious concern. The early clinical similarity of MPXV to common ailments like the flu and cold, coupled with the resemblances of its progressing rash to other infections, underscores the importance of prompt and accurate diagnosis. Among the infections, smallpox is clinically closest to MPXV, and rashes similar to MPXV stages also appear in syphilis and varicella zoster. A comprehensive review of MPXV, herpes, and syphilis was carried out, including structural and morphological features, origins, transmission modes, and computational studies. PubMed literature search on MPXV, using MeSH key terms, yielded 1904 results, with the analysis revealing prominent links to sexually transmitted diseases. More in-depth exploration of MPXV, Herpes Simplex Virus (HSV), and Syphilis revealed further disease interconnections and geographical correlations. These findings emphasize the need for a holistic understanding of these interconnected infectious agents for better control and management.
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  • 文章类型: Journal Article
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  • 文章类型: Journal Article
    抑制人巨细胞病毒(HCMV)立即早期(IE)基因表达是建立和维持潜伏储库的关键调控步骤。通过用组蛋白去乙酰化酶抑制剂如丙戊酸(VPA)治疗,病毒IE转录和蛋白质积累可以在潜伏期提高,使感染的细胞对适应性免疫反应可见。然而,潜伏期相关病毒蛋白UL138在支持潜伏期的不完全分化骨髓细胞感染期间抑制VPA增强IE基因表达的能力.UL138还通过抑制cGAS-STING-TBK1DNA传感途径来限制IFNβ转录物的积累。这里,我们证明,在不存在UL138的情况下,cGAS-STING-TBK1途径在不完全分化的骨髓细胞中促进IFNβ积累和VPA反应性IE基因表达。通过遗传或药理抑制使这一途径失活,表现出UL138表达并减少VPA反应性IE转录物和蛋白质积累。这项工作揭示了细胞质病原体传感和病毒裂解期转录的表观遗传控制之间的联系,并表明模式识别受体信号通路的操纵可以帮助MIEP调节策略的细化,以靶向潜伏的病毒储库。
    Repression of human cytomegalovirus (HCMV) immediate-early (IE) gene expression is a key regulatory step in the establishment and maintenance of latent reservoirs. Viral IE transcription and protein accumulation can be elevated during latency by treatment with histone deacetylase inhibitors such as valproic acid (VPA), rendering infected cells visible to adaptive immune responses. However, the latency-associated viral protein UL138 inhibits the ability of VPA to enhance IE gene expression during infection of incompletely differentiated myeloid cells that support latency. UL138 also limits the accumulation of IFNβ transcripts by inhibiting the cGAS-STING-TBK1 DNA-sensing pathway. Here, we show that, in the absence of UL138, the cGAS-STING-TBK1 pathway promotes both IFNβ accumulation and VPA-responsive IE gene expression in incompletely differentiated myeloid cells. Inactivation of this pathway by either genetic or pharmacological inhibition phenocopied UL138 expression and reduced VPA-responsive IE transcript and protein accumulation. This work reveals a link between cytoplasmic pathogen sensing and epigenetic control of viral lytic phase transcription and suggests that manipulation of pattern recognition receptor signaling pathways could aid in the refinement of MIEP regulatory strategies to target latent viral reservoirs.
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  • 文章类型: Journal Article
    最近癌症免疫疗法的成功,如免疫检查点抑制剂(ICIs),单克隆抗体(mAb),癌症疫苗,和过继细胞疗法(ACTs),彻底改变了传统的癌症治疗方法。然而,这些免疫治疗方式具有可变的功效,其中许多都表现出不良影响。溶瘤病毒免疫治疗(OViT),利用病毒直接或间接诱导抗癌免疫反应,正在成为治疗不同类型癌症患者的新型免疫疗法。1型单纯疱疹病毒(HSV-1)具有许多特征,可作为有效的OViT药物使用,并且仍然是主要的候选药物。其最近的临床成功导致美国食品和药物管理局(FDA)于2015年批准了Talimogenelaherparevec(T-VEC或Immygic)用于治疗晚期黑色素瘤。在这次审查中,我们讨论了基于溶瘤HSV-1的OViTs的开发的最新进展,它们的抗肿瘤作用机制,和近期临床试验的疗效数据。我们设想这些知识可用于指导未来oHSV在癌症治疗中的合理设计和应用。
    The recent success of cancer immunotherapies, such as immune checkpoint inhibitor (ICIs), monoclonal antibodies (mAbs), cancer vaccines, and adoptive cellular therapies (ACTs), has revolutionized traditional cancer treatment. However, these immunotherapeutic modalities have variable efficacies, and many of them exhibit adverse effects. Oncolytic viral Immunotherapy (OViT), whereby viruses are used to directly or indirectly induce anti-cancer immune responses, is emerging as a novel immunotherapy for treating patients with different types of cancer. The herpes simplex virus type-1 (HSV-1) possesses many characteristics that inform its use as an effective OViT agents and remains a leading candidate. Its recent clinical success resulted in the Food and Drug Administration (FDA) approval of Talimogene laherparevec (T-VEC or Imlygic) in 2015 for the treatment of advanced melanoma. In this review, we discuss recent advances in the development of oncolytic HSV-1-based OViTs, their anti-tumor mechanism of action, and efficacy data from recent clinical trials. We envision this knowledge may be used to inform the rational design and application of future oHSV in cancer treatment.
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  • 文章类型: Journal Article
    背景:人类单纯疱疹病毒(HSV)株HSV-1和HSV-2的妊娠相关感染尤其值得注意。有许多报道的疱疹感染的产时传播的例子,尽管从母亲到胎儿的宫内转移极为罕见。这项研究的目的是评估罗马尼亚西部地区孕妇中HSV-1和HSV-2抗体的血清阳性率。
    方法:将2013年至2016年,2019年至2022年在罗马尼亚克拉约瓦县临床急诊医院接受常规妊娠监测的孕妇纳入研究。为了寻找抗HSV-1/2IgG抗体,我们对患者进行了血清学检测,并收集了他们的人口统计信息.
    结果:HSV-1血清阳性率在农村地区有所下降,在城市地区有所上升,2013年至2016年的数值为89.30%,2019年至2022年的数值为84.96%,分别。35岁以上孕妇的血清阳性率最高。HSV-2的血清阳性率从2013-2016年的16.16%下降到2019-2022年的12.43%,农村和城市地区继续经历这种下降趋势。同样,35岁以上的孕妇感染HSV-1的频率最高.
    结论:通过了解HSV-1和HSV-2感染的血清阳性率,可以更容易地制定教育计划和采取其他行动来降低传播率并最终降低疾病的患病率。
    BACKGROUND: Pregnancy-related infections with the human herpes simplex virus (HSV) strains HSV-1 and HSV-2 are particularly noteworthy. There are numerous reported examples of intrapartum transmission of herpes infection, notwithstanding the extreme rarity of intrauterine transfer from mother to fetus. The purpose of this study was to evaluate the seroprevalence of HSV-1 and HSV-2 antibodies in pregnant women in the western region of Romania.
    METHODS: Pregnant women who presented for routine pregnancy monitoring at Romania\'s County Clinical Emergency Hospital in Craiova between 2013 and 2016 and 2019 and 2022 were included in the study. In order to find anti-HSV-1/2 IgG antibodies, we conducted serological testing on the patients and gathered demographic information from them.
    RESULTS: HSV-1 seroprevalence was shown to have declined in rural areas and increased in urban areas, with values between 2013 and 2016 being 89.30% and those between 2019 and 2022 being 84.96%, respectively. Women over 35 who were pregnant had the highest seroprevalence. The seroprevalence of HSV-2 decreased from 16.16% in 2013-2016 to 12.43% in 2019-2022, and both rural and urban areas continued to experience this declining trend. Similarly, pregnant women over 35 years old had the highest frequency of HSV-1 infections.
    CONCLUSIONS: Establishing educational programs and other actions to reduce the transmission rate and ultimately the prevalence of the disease can be made easier with knowledge about the seroprevalence of HSV-1 and HSV-2 infections.
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  • 文章类型: Journal Article
    获得对抗病毒药物的抗性是抗微生物治疗中的重要问题。为了鉴定新的抗病毒化合物,研究了匈牙利南部地区8种植物对单纯疱疹病毒2(HSV-2)的抗病毒活性。测试了植物提取物和植物化合物鼠尾草酸对Vero和HeLa细胞上HSV-2的细胞外和细胞内形式的有效性。通过直接定量PCR(qPCR)测量HSV-2复制。在测试的植物提取物中,丹参迷迭香(S.迷迭香)在0.47μg/mL浓度下显示HSV-2复制减少90.46%。鼠尾草酸,迷迭香中发现的一种主要抗菌化合物,还证明了对HSV-2的细胞外和细胞内形式的显著剂量依赖性抑制。鼠尾草酸的90%抑制浓度(IC90)为25-6.25μg/mL。蛋白质组学和高分辨率呼吸测定表明,鼠尾草酸抑制关键的ATP合成途径,如糖酵解,柠檬酸盐循环,和氧化磷酸化。氧化磷酸化的抑制也抑制HSV-2复制高达39.94倍。这些结果表明鼠尾草酸的抗病毒作用包括通过抑制关键能量产生途径来抑制ATP产生。鼠尾草酸有望成为针对HSV-2的潜在新型抗病毒剂。
    Acquiring resistance against antiviral drugs is a significant problem in antimicrobial therapy. In order to identify novel antiviral compounds, the antiviral activity of eight plants indigenous to the southern region of Hungary against herpes simplex virus-2 (HSV-2) was investigated. The plant extracts and the plant compound carnosic acid were tested for their effectiveness on both the extracellular and intracellular forms of HSV-2 on Vero and HeLa cells. HSV-2 replication was measured by a direct quantitative PCR (qPCR). Among the tested plant extracts, Salvia rosmarinus (S. rosmarinus) exhibited a 90.46% reduction in HSV-2 replication at the 0.47 μg/mL concentration. Carnosic acid, a major antimicrobial compound found in rosemary, also demonstrated a significant dose-dependent inhibition of both extracellular and intracellular forms of HSV-2. The 90% inhibitory concentration (IC90) of carnosic acid was between 25 and 6.25 μg/mL. Proteomics and high-resolution respirometry showed that carnosic acid suppressed key ATP synthesis pathways such as glycolysis, citrate cycle, and oxidative phosphorylation. Inhibition of oxidative phosphorylation also suppressed HSV-2 replication up to 39.94-fold. These results indicate that the antiviral action of carnosic acid includes the inhibition of ATP generation by suppressing key energy production pathways. Carnosic acid holds promise as a potential novel antiviral agent against HSV-2.
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