papillomavirus

乳头瘤病毒
  • 文章类型: Journal Article
    Human papillomaviruses (HPVs) infect cutaneous and mucosal epithelia to cause benign (warts) and malignant lesions (e.g. cervical cancer). Bovine papillomaviruses (BPVs) infect fibroblasts to cause fibropapillomas but can also infect cutaneous epithelial cells. For HPV-1, -16, -31 and BPV-1, cis-acting RNA elements in the late 3\' untranslated region (3\'UTR) control expression of virus proteins by binding host cell proteins. The present study compared the effects on gene expression of the cis-acting elements of seven PV late 3\'UTRs (HPV-6b, -11, -16, -31 and BPV-1, -3 and -4) representing a range of different genera and species and pathological properties. pSV-beta-galactosidase reporter plasmids containing the late 3\'UTRs from seven PVs were transiently transfected into cervical adenocarcinoma HeLa cells, and reporter gene expression quantified by reverse transcription-quantitative PCR and a beta-galactosidase assay. All elements inhibited gene expression in keratinocytes. Cancer-related types HPV-16 and -31, had the greatest inhibitory activity whereas the lowest inhibition was found in the non-cancer related types, BPV-3 and HPV-11. Using RBPmap version 1.1, bioinformatics predictions of factors binding the elements identified proteins which function mainly in mRNA splicing. Markedly, in terms of protein binding motifs, BPV late 3\'UTR elements were similar to those of HPV-1a but not to other HPVs. Using HPV-1a as a model and siRNA depletion, the bioinformatics predictions were tested and it was found that PABPC4 was responsible for some of the 3\'UTR repressive activity. The data revealed candidate proteins that could control PV late gene expression.
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  • 文章类型: Journal Article
    背景:乳头状瘤DNA病毒是引起反刍动物皮肤损伤的病毒之一。
    目的:临床,本研究将研究伊朗反刍动物皮肤乳头状瘤的组织病理学和分子特征。
    方法:从具有各种乳头状瘤病病变的19只小反刍动物(5只绵羊和14只山羊)中收集样本。用组织病理学和分子技术研究了所采集的样品。
    结果:在临床方面,病变大小不同,范围从0.5到11厘米,花椰菜的外生肿块出现在动物身体的其他部位。在四肢,已见到大多数乳头状瘤病变(42.1%)。在组织病理学检查中,核周空泡化表皮颗粒层具有不同程度的高颗粒病,角化过度,棘皮病,可见角膜塑形和角化不全。此外,使用聚合酶链反应技术,所有疑似样本的乳头状瘤病毒均呈阳性.
    结论:尽管伊朗绵羊和山羊中乳头状瘤病毒的流行率很低,似乎有必要将它们与其他病毒性皮肤病区分开来,如皮肤传染性的湿疹,使用分子技术和组织病理学。
    BACKGROUND: Papilloma DNA viruses are one of the viruses that cause skin lesions in ruminants.
    OBJECTIVE: The clinical, histopathological and molecular characteristics of cutaneous papilloma in ruminants in Iran are to be investigated in this study.
    METHODS: Samples were collected from 19 small ruminants (5 sheep and 14 goats) with various papillomatosis lesions. The samples taken were studied with histopathological and molecular techniques.
    RESULTS: In clinical terms, the lesions appeared in different sizes, ranging from 0.5 to 11 cm, and the cauliflower exophytic masses appeared in other parts of the animal\'s body. In the limbs, most papilloma lesions have been seen (42.1%). In histopathological examination, perinuclear vacuolation epidermal granule layer with various degrees of hypergranulosis, hyperkeratosis, acanthosis, orthokeratosis and parakeratosis were seen. Moreover, all the suspected samples were positive for papillomavirus using the polymerase chain reaction technique.
    CONCLUSIONS: Although the prevalence of papillomaviruses in Iranian sheep and goats is low, it seems necessary to distinguish them from other viral skin diseases, such as cutaneous contagious ecthyma, using molecular techniques and histopathology.
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  • 文章类型: Journal Article
    产生持续感染的DNA病毒被认为是尼安德特人灭绝的潜在原因,and,因此,尼安德特人序列读段中病毒基因组残留物的鉴定是解决这一假设的第一步.这里,作为概念的证明,我们通过绘制腺病毒来搜索尼安德特人基因组数据序列中的病毒残留物,疱疹病毒和乳头状瘤病毒,它们是双链DNA病毒,可以建立终身潜伏期,并可以产生持续的感染。重建的腺病毒古老的病毒基因组,疱疹病毒和乳头状瘤病毒揭示了保守的片段,与现存的病毒基因组和编码区的可变区具有核苷酸同一性,与现存的近亲有很大的分歧。映射到现有病毒基因组的序列读数显示了古代DNA的脱氨基模式,这些古老的病毒基因组显示出与这些样本的年龄(约50,000年)和病毒进化率(10-5至10-8个替换/位点/年)一致的差异。随机效应的分析表明,尼安德特人对现有持久性病毒基因组的映射高于短读段的随机相似性所预期的。此外,使用非持久性DNA病毒的阴性对照不产生统计学上显著的装配。这项工作证明了通过信噪比评估来识别考古样本中病毒基因组残留物的可行性。
    DNA viruses that produce persistent infections have been proposed as potential causes for the extinction of Neanderthals, and, therefore, the identification of viral genome remnants in Neanderthal sequence reads is an initial step to address this hypothesis. Here, as proof of concept, we searched for viral remnants in sequence reads of Neanderthal genome data by mapping to adenovirus, herpesvirus and papillomavirus, which are double-stranded DNA viruses that may establish lifelong latency and can produce persistent infections. The reconstructed ancient viral genomes of adenovirus, herpesvirus and papillomavirus revealed conserved segments, with nucleotide identity to extant viral genomes and variable regions in coding regions with substantial divergence to extant close relatives. Sequence reads mapped to extant viral genomes showed deamination patterns of ancient DNA, and these ancient viral genomes showed divergence consistent with the age of these samples (≈50,000 years) and viral evolutionary rates (10-5 to 10-8 substitutions/site/year). Analysis of random effects showed that the Neanderthal mapping to genomes of extant persistent viruses is above what is expected by random similarities of short reads. Also, negative control with a nonpersistent DNA virus does not yield statistically significant assemblies. This work demonstrates the feasibility of identifying viral genome remnants in archaeological samples with signal-to-noise assessment.
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  • 文章类型: Journal Article
    天津发生了一场关于养殖中国舌底的大规模死亡事件,中国,病原体仍然未知。这里,通过电子显微镜从患病的鱼中同时分离并鉴定了一种新型的半乳头瘤病毒(CsPaV)和细小病毒(CsPV),病毒分离,基因组测序,实验挑战,和荧光原位杂交(FISH)。电子显微镜显示,患病鱼的组织中存在大量病毒颗粒。在比目鱼g细胞(FG)中分离和繁殖的病毒会诱导典型的细胞病变效应(CPE)。给予腹膜内注射的鱼的累积死亡率在7dpi时达到100%。CsPaV和CsPV的完整基因组包括5939bp和3663bp,分别,基因组与其他病毒没有核苷酸序列相似性。基于L1和NS1蛋白序列的系统发育分析表明,CsPaV和CsPV是乳头状病毒科和细小病毒科的新成员。FISH结果显示感染鱼的脾脏组织中存在阳性信号,两种病毒都可以共同感染单个细胞。这项研究代表了在养殖海洋养殖鱼类中发现新型乳头瘤病毒和细小病毒的第一份报告,为进一步研究新发病毒性疾病的防治提供了依据。
    A massive mortality event concerning farmed Chinese tongue soles occurred in Tianjin, China, and the causative agent remains unknown. Here, a novel Cynoglossus semilaevis papillomavirus (CsPaV) and parvovirus (CsPV) were simultaneously isolated and identified from diseased fish via electron microscopy, virus isolation, genome sequencing, experimental challenges, and fluorescence in situ hybridization (FISH). Electron microscopy showed large numbers of virus particles present in the tissues of diseased fish. Viruses that were isolated and propagated in flounder gill cells (FG) induced typical cytopathic effects (CPE). The cumulative mortality of fish given intraperitoneal injections reached 100% at 7 dpi. The complete genomes of CsPaV and CsPV comprised 5939 bp and 3663 bp, respectively, and the genomes shared no nucleotide sequence similarities with other viruses. Phylogenetic analysis based on the L1 and NS1 protein sequences revealed that CsPaV and CsPV were novel members of the Papillomaviridae and Parvoviridae families. The FISH results showed positive signals in the spleen tissues of infected fish, and both viruses could co-infect single cells. This study represents the first report where novel papillomavirus and parvovirus are identified in farmed marine cultured fish, and it provides a basis for further studies on the prevention and treatment of emerging viral diseases.
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  • 文章类型: Journal Article
    建议接种人乳头瘤病毒(HPV)疫苗以避免HPV感染及其相关疾病,包括宫颈癌.然而,孟加拉国人口中没有意识研究。因此,这项全国性研究旨在探讨符合条件的青春期女孩父母对HPV疫苗的知晓率及其决定因素.
    这项研究是在6月28日至2023年8月2日期间,在孟加拉国64个随机选择的地区中,有42个地区的9-15岁女儿的父母中进行的。使用多阶段抽样方法从孟加拉国所有八个部门招募2151名研究参与者。本研究采用半结构化问卷进行面对面访谈。使用统计软件Stata(版本17)进行统计分析。
    参与者的平均年龄为38.18(±5.86)岁。只有22.32%的参与者知道HPV疫苗。年龄每增加一年,知道HPV疫苗的可能性就会增加3%(AOR:1.03;95CI:1.00-1.06)。居住在城市地区的参与者的意识几率是农村和半城市人群的3.56倍。与工作人员相比,商人和家庭主妇的赔率较低60%(AOR:0.40;95%CI:0.22-0.69)和77%(AOR:0.23;95%CI:0.16-0.33)。与中等收入和高收入组相比,低收入组表现出明显更高的意识几率(AOR:0.25,95CI:0.16-0.39)。从未接受过常规健康检查的参与者比接受过常规健康检查的参与者意识到的几率低77%(AOR:0.23;95CI:0.16-0.34)。
    孟加拉国普通人群对HPV疫苗的认识非常低。年龄,residence,职业,月收入,常规体检与HPV疫苗意识相关.在全国范围内开展提高认识运动将提高孟加拉国人口的这一认识水平,尤其是女儿的父母。
    UNASSIGNED: Vaccination against Human papillomavirus (HPV) is recommended to avoid HPV infections and its associated diseases, including cervical cancer. However, there is no awareness study among Bangladeshi population. Hence, this nationwide study was conducted to explore HPV vaccine awareness and its determinants among parents of eligible adolescent girls.
    UNASSIGNED: This study was conducted among the parents of daughters aged 9-15 years from 42 out of 64 randomly selected districts of Bangladesh between June 28 to August 2, 2023. A multistage sampling method was used to enroll 2151 study participants from all eight divisions of Bangladesh. A semi-structured questionnaire was used for face-to-face interviews in this study. The statistical software Stata (Version 17) was used for statistical analyses.
    UNASSIGNED: The average age of the participants was 38.18 (±5.86) years. Only 22.32 % of the participants were aware of the HPV vaccine. Every additional year of age increased the likelihood of being aware of the HPV vaccine by 3 % (AOR: 1.03; 95%CI: 1.00-1.06). Participants residing in the urban area had 3.56 times higher odds of awareness than rural and semi-urban people. Businessmen and housewives had 60 % (AOR: 0.40; 95 % CI: 0.22-0.69) and 77 % (AOR: 0.23; 95 % CI: 0.16-0.33) lower odds in comparison to job holders. The lower-income group exhibited significantly higher odds of awareness (AOR: 0.25, 95%CI: 0.16-0.39) compared to the middle and the higher-income group. Participants who never went through routine health check-ups had 77 % lower odds of being aware than those who availed of regular routine check-ups (AOR: 0.23; 95%CI: 0.16-0.34).
    UNASSIGNED: Awareness of the HPV vaccine among the general population of Bangladesh is very low. Age, residence, occupation, monthly income, and routine medical check-ups were associated with HPV vaccine awareness. A nationwide awareness campaign would increase this awareness level among the Bangladeshi population, especially among the parents of daughters.
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  • 文章类型: Journal Article
    人乳头瘤病毒(HPV)是美国最常见的性传播感染,是肛门生殖道和口腔癌的主要病因。越来越多的证据表明,宿主微生物组的变化与HPV感染的自然史和最终结果有关。我们试图定义乳头瘤病毒感染期间宿主宫颈阴道微生物组的变化,持久性,和发病机制使用小鼠乳头瘤病毒(MmuPV1)宫颈阴道感染模型。在具有免疫能力的雌性FVB/N小鼠中MmuPV1感染的时间过程中进行宫颈阴道灌洗,并通过qPCR分析提取的DNA以跟踪MmuPV1病毒拷贝数。16S核糖体RNA(rRNA)基因测序用于确定整个时间过程中微生物群落的组成和多样性。我们还试图确定特定的微生物群落是否存在于MmuPV1诱导的肿瘤性疾病的范围内。我们,因此,进行激光捕获显微切割,以分离代表肿瘤疾病进展所有阶段的疾病区域(正常,低级和高级发育不良,和癌症)来自MmuPV1感染小鼠的雌性生殖道组织切片,并进行了16SrRNA测序。与其他研究一致,我们发现,天然小鼠宫颈阴道微生物组在不同的实验中是高度可变的。尽管实验之间的初始微生物组组成存在差异,我们观察到MmuPV1持久性,病毒载量,和疾病的严重程度影响宫颈阴道微生物组的组成。这些研究表明,乳头瘤病毒感染可以改变宫颈阴道微生物组。重要的人乳头瘤病毒(HPVs)是美国最常见的性传播感染。感染肛门生殖道的HPV子集(子宫颈,阴道,肛门)和口腔导致全球至少5%的癌症。最近的证据表明,存在于人类子宫颈和阴道中的微生物群落,被称为宫颈阴道微生物组,在HPV诱导的宫颈癌中起作用。然而,这种相互作用背后的机制并不明确。在这项研究中,我们用小鼠乳头瘤病毒(MmuPV1)感染小鼠的雌性生殖道,发现乳头瘤病毒感染和疾病的关键方面影响宿主宫颈阴道微生物组。这是第一项在HPV诱导的宫颈癌的临床前动物模型中定义与MmuPV1感染相关的宿主微生物组变化的研究。这些结果为使用MmuPV1感染模型进一步研究乳头状瘤病毒与宿主微生物组之间的相互作用铺平了道路。
    Human papillomaviruses (HPVs) are the most common sexually transmitted infection in the United States and are a major etiological agent of cancers in the anogenital tract and oral cavity. Growing evidence suggests changes in the host microbiome are associated with the natural history and ultimate outcome of HPV infection. We sought to define changes in the host cervicovaginal microbiome during papillomavirus infection, persistence, and pathogenesis using the murine papillomavirus (MmuPV1) cervicovaginal infection model. Cervicovaginal lavages were performed over a time course of MmuPV1 infection in immunocompetent female FVB/N mice and extracted DNA was analyzed by qPCR to track MmuPV1 viral copy number. 16S ribosomal RNA (rRNA) gene sequencing was used to determine the composition and diversity of microbial communities throughout this time course. We also sought to determine whether specific microbial communities exist across the spectrum of MmuPV1-induced neoplastic disease. We, therefore, performed laser-capture microdissection to isolate regions of disease representing all stages of neoplastic disease progression (normal, low- and high-grade dysplasia, and cancer) from female reproductive tract tissue sections from MmuPV1-infected mice and performed 16S rRNA sequencing. Consistent with other studies, we found that the natural murine cervicovaginal microbiome is highly variable across different experiments. Despite these differences in initial microbiome composition between experiments, we observed that MmuPV1 persistence, viral load, and severity of disease influenced the composition of the cervicovaginal microbiome. These studies demonstrate that papillomavirus infection can alter the cervicovaginal microbiome.IMPORTANCEHuman papillomaviruses (HPVs) are the most common sexually transmitted infection in the United States. A subset of HPVs that infect the anogenital tract (cervix, vagina, anus) and oral cavity cause at least 5% of cancers worldwide. Recent evidence indicates that the community of microbial organisms present in the human cervix and vagina, known as the cervicovaginal microbiome, plays a role in HPV-induced cervical cancer. However, the mechanisms underlying this interplay are not well-defined. In this study, we infected the female reproductive tract of mice with a murine papillomavirus (MmuPV1) and found that key aspects of papillomavirus infection and disease influence the host cervicovaginal microbiome. This is the first study to define changes in the host microbiome associated with MmuPV1 infection in a preclinical animal model of HPV-induced cervical cancer. These results pave the way for using MmuPV1 infection models to further investigate the interactions between papillomaviruses and the host microbiome.
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  • 文章类型: Journal Article
    人乳头瘤病毒16(HPV16)E2与细胞蛋白TopBP1和BRD4之间的相互作用是E2质粒分离功能所必需的。E2-TopBP1相互作用促进U2OS和N/Tert-1细胞中有丝分裂E2蛋白水平增加,以及通过HPV16(HFKHPV16)永生化的人包皮角质形成细胞。SIRT1脱乙酰化降低E2蛋白的稳定性,在这里我们证明了在有丝分裂过程中E2乙酰化的增加以TopBP1相互作用依赖性方式发生。促进E2有丝分裂稳定。p300介导E2乙酰化和乙酰化增加,由于E2在有丝分裂过程中以TopBP1相互作用依赖性方式关闭SIRT1功能,通过增加的p53稳定性和赖氨酸382的乙酰化,SIRT1去乙酰化的已知目标证实。SIRT1可以在生长中的细胞中与E2复合,但由于E2-TopBP1相互作用,在有丝分裂期间无法这样做;SIRT1也无法在有丝分裂E2野生型细胞中与p53复合,但可以在有丝分裂之外与p53复合。E2赖氨酸111和112是所有E2蛋白中高度保守的残基,我们证明了K111在有丝分裂过程中发生过度乙酰化,促进E2与拓扑异构酶1(Top1)的相互作用。我们证明K112泛素化促进有丝分裂过程中的E2蛋白酶体降解。E2-TopBP1相互作用促进CHK2的有丝分裂乙酰化,促进DNA损伤反应(DDR)的磷酸化和激活。结果提出了一种新的模型,其中E2-TopBP1复合物在有丝分裂期间使SIRT1失活,并激活DDR。这是一种新的HPV16激活DDR的机制,病毒生命周期的要求。
    目的:人类乳头瘤病毒(HPV)是所有人类癌症中约5%的病原体。虽然有预防性疫苗可以显著减轻后代的HPV疾病负担,目前尚无抗病毒策略可用于治疗HPV癌症.为了产生这样的试剂,我们必须更多地了解HPV的生命周期,特别是关于病毒与宿主的相互作用。这里,我们描述了由HPV16E2蛋白与控制脱乙酰酶SIRT1功能的宿主蛋白TopBP1相互作用产生的新型有丝分裂复合物。E2-TopBP1相互作用在有丝分裂期间破坏SIRT1功能,以增强病毒和宿主蛋白的乙酰化和稳定性。我们还证明E2-TopBP1相互作用激活DDR。这种新型复合物对于HPV16生命周期是必不可少的,并且代表了一种新型的抗病毒治疗靶标。
    An interaction between human papillomavirus 16 (HPV16) E2 and the cellular proteins TopBP1 and BRD4 is required for E2 plasmid segregation function. The E2-TopBP1 interaction promotes increased mitotic E2 protein levels in U2OS and N/Tert-1 cells, as well as in human foreskin keratinocytes immortalized by HPV16 (HFK + HPV16). SIRT1 deacetylation reduces E2 protein stability and here we demonstrate that increased E2 acetylation occurs during mitosis in a TopBP1 interacting-dependent manner, promoting E2 mitotic stabilization. p300 mediates E2 acetylation and acetylation is increased due to E2 switching off SIRT1 function during mitosis in a TopBP1 interacting-dependent manner, confirmed by increased p53 stability and acetylation on lysine 382, a known target for SIRT1 deacetylation. SIRT1 can complex with E2 in growing cells but is unable to do so during mitosis due to the E2-TopBP1 interaction; SIRT1 is also unable to complex with p53 in mitotic E2 wild-type cells but can complex with p53 outside of mitosis. E2 lysines 111 and 112 are highly conserved residues across all E2 proteins and we demonstrate that K111 hyper-acetylation occurs during mitosis, promoting E2 interaction with Topoisomerase 1 (Top1). We demonstrate that K112 ubiquitination promotes E2 proteasomal degradation during mitosis. E2-TopBP1 interaction promotes mitotic acetylation of CHK2, promoting phosphorylation and activation of the DNA damage response (DDR). The results present a new model in which the E2-TopBP1 complex inactivates SIRT1 during mitosis, and activates the DDR. This is a novel mechanism of HPV16 activation of the DDR, a requirement for the viral life cycle.
    OBJECTIVE: Human papillomaviruses (HPVs) are causative agents in around 5% of all human cancers. While there are prophylactic vaccines that will significantly alleviate HPV disease burden on future generations, there are currently no anti-viral strategies available for the treatment of HPV cancers. To generate such reagents, we must understand more about the HPV life cycle, and in particular about viral-host interactions. Here, we describe a novel mitotic complex generated by the HPV16 E2 protein interacting with the host protein TopBP1 that controls the function of the deacetylase SIRT1. The E2-TopBP1 interaction disrupts SIRT1 function during mitosis in order to enhance acetylation and stability of viral and host proteins. We also demonstrate that the E2-TopBP1 interaction activates the DDR. This novel complex is essential for the HPV16 life cycle and represents a novel anti-viral therapeutic target.
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  • 文章类型: Preprint
    这项研究的最初目的是通过分析公开可用的深度测序数据集的从头组装来阐明小DNA肿瘤病毒的进化。该调查生成了一个可搜索的重叠群快照数据库,代表100,000多个序列读取存档记录。使用现代结构感知搜索工具,我们反复扩大搜索范围,以包括越来越广泛的其他病毒家族。分析揭示了令人惊讶的不同范围的嵌合体,涉及不同的病毒组。在某些情况下,类似于已知DNA复制模块或已知病毒体蛋白操纵子的基因与无法识别的序列配对,结构预测表明这些序列可能代表以前未知的复制酶和新型病毒体结构。在代表人类和其他灵长类动物的数据集中发现了一个新兴群体的离散进化枝,称为腺体病毒。作为概念的证明,我们表明,重叠群数据库也可用于发现RNA病毒和候选古细菌噬菌体。辅助搜索揭示了不同病毒组之间嵌合的其他实例。这些观察结果支持以基因为中心的分类学框架,该框架应该对未来的病毒狩猎工作有用。
    The initial objective of this study was to shed light on the evolution of small DNA tumor viruses by analyzing de novo assemblies of publicly available deep sequencing datasets. The survey generated a searchable database of contig snapshots representing more than 100,000 Sequence Read Archive records. Using modern structure-aware search tools, we iteratively broadened the search to include an increasingly wide range of other virus families. The analysis revealed a surprisingly diverse range of chimeras involving different virus groups. In some instances, genes resembling known DNA-replication modules or known virion protein operons were paired with unrecognizable sequences that structural predictions suggest may represent previously unknown replicases and novel virion architectures. Discrete clades of an emerging group called adintoviruses were discovered in datasets representing humans and other primates. As a proof of concept, we show that the contig database is also useful for discovering RNA viruses and candidate archaeal phages. The ancillary searches revealed additional examples of chimerization between different virus groups. The observations support a gene-centric taxonomic framework that should be useful for future virus-hunting efforts.
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  • 文章类型: Journal Article
    FMS相关酪氨酸激酶3配体(FLT3L),由FLT3LG编码,是自然杀伤(NK)细胞发育所必需的造血因子,B细胞,和小鼠中的树突状细胞(DC)。我们描述了三个人类纯合的功能丧失FLT3LG变体,具有各种复发性感染的历史,包括严重的皮肤疣.患者骨髓(BM)发育不良,造血祖细胞水平低,特别是骨髓和B细胞前体。B细胞计数,单核细胞,患者血液中的DCs很低,而其他血液亚群,包括NK细胞,只受到中度影响,如果有的话。患者皮肤中的朗格汉斯细胞(LC)和真皮巨噬细胞计数正常,但缺乏真皮DC。因此,FLT3L是小鼠和人类B细胞和DC发育所必需的。然而,与鼠类不同,人FLT3L是单核细胞而不是NK细胞发育所必需的。
    FMS-related tyrosine kinase 3 ligand (FLT3L), encoded by FLT3LG, is a hematopoietic factor essential for the development of natural killer (NK) cells, B cells, and dendritic cells (DCs) in mice. We describe three humans homozygous for a loss-of-function FLT3LG variant with a history of various recurrent infections, including severe cutaneous warts. The patients\' bone marrow (BM) was hypoplastic, with low levels of hematopoietic progenitors, particularly myeloid and B cell precursors. Counts of B cells, monocytes, and DCs were low in the patients\' blood, whereas the other blood subsets, including NK cells, were affected only moderately, if at all. The patients had normal counts of Langerhans cells (LCs) and dermal macrophages in the skin but lacked dermal DCs. Thus, FLT3L is required for B cell and DC development in mice and humans. However, unlike its murine counterpart, human FLT3L is required for the development of monocytes but not NK cells.
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  • 文章类型: Journal Article
    幼年发作的复发性呼吸道乳头状瘤是与HPV感染相关的终生良性鳞状病变,特别是HPV6和HPV11基因型。这些病变很罕见,但是会导致喉阻塞,会导致呼吸困难,或者转变成鳞状细胞癌.这里的目的是提供一种流行病学,这种病理学的生物学和临床概述,特别是在儿童中,为了了解在研究和开发医疗和治疗管理工具方面的问题。
    Juvenile onset recurrent respiratory papillomatosis is a lifelong benign squamous lesion associated with HPV infection, particularly HPV6 and HPV11 genotypes. These lesions are rare, but can lead to laryngeal obturations, which can cause disabling dyspnea, or transform into squamous cell carcinoma. The aim here is to provide an epidemiological, biological and clinical overview of this pathology, particularly in children, in order to understand the issues at stake in terms of research and the development of medical and therapeutic management tools.
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