Bolstering the Number and Function of HSV-1–Specific CD8+ Effector Memory T Cells and Tissue-Resident Memory T Cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease

Arif A. Khan; Ruchi Srivastava; Aziz A. Chentoufi; Elizabeth Kritzer; Sravya Chilukuri; Sumit Garg; David C. Yu; Hawa Vahed; Lei Huang; Sabrina A. Syed; Julie N. Furness; Tien T. Tran; Nesburn B. Anthony; Christine E. McLaren; John Sidney; Alessandro Sette; Randolph J. Noelle; Lbachir BenMohamed

首页> 外文期刊>The journal of immunology >Bolstering the Number and Function of HSV-1–Specific CD8+ Effector Memory T Cells and Tissue-Resident Memory T Cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease

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Bolstering the Number and Function of HSV-1–Specific CD8+ Effector Memory T Cells and Tissue-Resident Memory T Cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease

机译：提高潜在感染的三叉神经节中HSV-1特异的CD8 +效应记忆T细胞和组织常驻T细胞的数量和功能可减少复发性眼疱疹感染和疾病

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HSV type 1 (HSV-1) is a prevalent human pathogen that infects 3.72 billion individuals worldwide and can cause potentially blinding recurrent corneal herpetic disease. HSV-1 establishes latency within sensory neurons of trigeminal ganglia (TG), and TG-resident CD8+ T cells play a critical role in preventing its reactivation. The repertoire, phenotype, and function of protective CD8+ T cells are unknown. Bolstering the apparent feeble numbers of CD8+ T cells in TG remains a challenge for immunotherapeutic strategies. In this study, a comprehensive panel of 467 HLA-A*0201–restricted CD8+ T cell epitopes was predicted from the entire HSV-1 genome. CD8+ T cell responses to these genome-wide epitopes were compared in HSV-1–seropositive symptomatic individuals (with a history of numerous episodes of recurrent herpetic disease) and asymptomatic (ASYMP) individuals (who are infected but never experienced any recurrent herpetic disease). Frequent polyfunctional HSV-specific IFN-γ+CD107a/b+CD44highCD62LlowCD8+ effector memory T cells were detected in ASYMP individuals and were primarily directed against three “ASYMP” epitopes. In contrast, symptomatic individuals have more monofunctional CD44highCD62LhighCD8+ central memory T cells. Furthermore, therapeutic immunization with an innovative prime/pull vaccine, based on priming with multiple ASYMP epitopes (prime) and neurotropic TG delivery of the T cell–attracting chemokine CXCL10 (pull), boosted the number and function of CD44highCD62LlowCD8+ effector memory T cells and CD103highCD8+ tissue-resident T cells in TG of latently infected HLA-A*0201–transgenic mice and reduced recurrent ocular herpes following UV-B–induced reactivation. These findings have profound implications in the development of T cell–based immunotherapeutic strategies to treat blinding recurrent herpes infection and disease.

机译：HSV 1型（HSV-1）是一种普遍存在的人类病原体，在全球范围内感染超过37.2亿个人，并可能导致复发性角膜疱疹疾病致盲。 HSV-1在三叉神经节（TG）的感觉神经元内建立潜伏期，而TG驻留的CD8 + T细胞在阻止其重新激活中起关键作用。保护性CD8 + T细胞的库，表型和功能尚不清楚。增强TG中CD8 + T细胞的表观微弱数量仍然是免疫治疗策略的挑战。在这项研究中，从整个HSV-1基因组中预测了467个HLA-A * 0201限制性CD8 + T细胞表位的全面组成。在HSV-1血清反应阳性的有症状个体（有多次复发性疱疹病史）和无症状（ASYMP）个体（被感染但从未经历过任何复发性疱疹病）中比较了对这些全基因组表位的CD8 + T细胞反应。在ASYMP个体中检测到常见的多功能HSV特异性IFN-γ+ CD107a / b + CD44highCD62LlowCD8 +效应记忆T细胞，并且主要针对三个“ ASYMP”表位。相反，有症状的个体具有更多的单功能CD44highCD62LhighCD8 +中枢记忆T细胞。此外，基于多种ASYMP表位（prime）的初免和吸引T细胞的趋化因子CXCL10（pull）的嗜神经性TG递送，创新的初免/拉动疫苗的治疗性免疫提高了CD44highCD62LlowCD8 +效应记忆T细胞和在潜伏感染的HLA-A * 0201转基因小鼠的TG中，CD103highCD8 +组织驻留性T细胞和UV-B诱导的激活后复发性眼疱疹减少。这些发现对基于T细胞的免疫疗法治疗盲目性复发性疱疹感染和疾病的战略发展具有深远的意义。

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《The journal of immunology》 |2017年第1期|共18页
作者
Arif A. Khan; Ruchi Srivastava; Aziz A. Chentoufi; Elizabeth Kritzer; Sravya Chilukuri; Sumit Garg; David C. Yu; Hawa Vahed; Lei Huang; Sabrina A. Syed; Julie N. Furness; Tien T. Tran; Nesburn B. Anthony; Christine E. McLaren; John Sidney; Alessandro Sette; Randolph J. Noelle; Lbachir BenMohamed;
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1. Bolstering the Number and Function of HSV-1-Specific CD8(+) Effector Memory T Cells and Tissue-Resident Memory T Cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease [J] . Khan Arif A., Srivastava Ruchi, Chentoufi Aziz A., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2017,第1期

机译：在潜在感染的三叉神经节中升压HSV-1特异性CD8（+）效应存储器T细胞和组织植物记忆T细胞的数量和功能可减少复发性眼疱感染和疾病
2. Circulating herpes simplex type 1 (HSV-1)-specific CD8+ T cells do not access HSV-1 latently infected trigeminal ganglia [J] . Susanne Himmelein, Anthony J St Leger, Jared E Knickelbein, Herpesviridae . 2011,第2期

机译：循环单纯疱疹1型（HSV-1）特异性CD8 + T细胞无法进入HSV-1潜伏感染的三叉神经节
3. Qa-1b and CD94-NKG2a Interaction Regulate Cytolytic Activity of Herpes Simplex Virus-Specific Memory CD8+ T Cells in the Latently Infected Trigeminal Ganglia [J] . Susmit Suvas, Ahmet Kursat Azkur, Barry T. Rouse The journal of immunology . 2006,第3期

机译：Qa-1b和CD94-NKG2a相互作用调节潜伏感染的三叉神经节中单纯疱疹病毒特异性记忆CD8 + T细胞的细胞溶解活性。
4. Memory CD8+ T Cells Remain Functional throughout an Ongoing Persistent Infection: Implications for Antigen-Specific Immune Reconstitution and Boosting. [D] . Quinn, Michael. 2017

机译：记忆CD8 + T细胞在持续的持续感染中仍保持功能性：对抗原特异性免疫重建和增强的影响。
5. Bolstering the Number and Function of HSV-1-Specific CD8+ TEM and TRM cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease [O] . Arif A. Khan, Ruchi Srivastava, Aziz A. Chentoufi, -1

机译：增强潜在感染的三叉神经节中HSV-1特异性CD8 + TEM和TRM细胞的数量和功能可减少复发性眼疱疹感染和疾病
6. Circulating herpes simplex type 1 (HSV-1)-specific CD8+ T cells do not access HSV-1 latently infected trigeminal ganglia [O] . Susanne Himmelein, Anthony J St Leger, Jared E Knickelbein, 2011

机译：循环单纯疱疹1型（HSV-1）特异的CD8 + T细胞无法进入HSV-1潜伏感染的三叉神经节

Bolstering the Number and Function of HSV-1–Specific CD8+ Effector Memory T Cells and Tissue-Resident Memory T Cells in Latently Infected Trigeminal Ganglia Reduces Recurrent Ocular Herpes Infection and Disease

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