Stress Signal ULBP4, an NKG2D Ligand, Is Upregulated in Multiple Sclerosis and Shapes CD8⁺ T-Cell Behaviors.

IF 7.5

Neurology(R) neuroimmunology & neuroinflammation Pub Date : 2021-12-06 Print Date: 2022-01-01 DOI:10.1212/NXI.0000000000001119

Ana Carmena Moratalla, Yves Carpentier Solorio, Florent Lemaitre, Negar Farzam-Kia, Annie Levert, Stephanie E J Zandee, Boaz Lahav, Jean Victor Guimond, Elie Haddad, Marc Girard, Pierre Duquette, Catherine Larochelle, Alexandre Prat, Nathalie Arbour

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引用次数: 4

Abstract

Background and objectives: We posit the involvement of the natural killer group 2D (NKG2D) pathway in multiple sclerosis (MS) pathology via the presence of specific NKG2D ligands (NKG2DLs). We aim to evaluate the expression of NKG2DLs in the CNS and CSF of patients with MS and to identify cellular stressors inducing the expression of UL16-binding protein 4 (ULBP4), the only detectable NKG2DL. Finally, we evaluate the impact of ULBP4 on functions such as cytokine production and motility by CD8⁺ T lymphocytes, a subset largely expressing NKG2D, the cognate receptor.

Methods: Human postmortem brain samples and CSF from patients with MS and controls were used to evaluate NKG2DL expression. In vitro assays using primary cultures of human astrocytes and neurons were performed to identify stressors inducing ULBP4 expression. Human CD8⁺ T lymphocytes from MS donors and age/sex-matched healthy controls were isolated to evaluate the functional impact of soluble ULBP4.

Results: We detected mRNA coding for the 8 identified human NKG2DLs in brain samples from patients with MS and controls, but only ULBP4 protein expression was detectable by Western blot. ULBP4 levels were greater in patients with MS, particularly in active and chronic active lesions and normal-appearing white matter, compared with normal-appearing gray matter from MS donors and white and gray matter from controls. Soluble ULBP4 was also detected in CSF of patients with MS and controls, but a smaller shed/soluble form of 25 kDa was significantly elevated in CSF from female patients with MS compared with controls and male patients with MS. Our data indicate that soluble ULBP4 affects various functions of CD8⁺ T lymphocytes. First, it enhanced the production of the proinflammatory cytokines GM-CSF and interferon-γ (IFNγ). Second, it increased CD8⁺ T lymphocyte motility and favored a kinapse-like behavior when cultured in the presence of human astrocytes. CD8⁺ T lymphocytes from patients with MS were especially altered by the presence of soluble ULBP4 compared with healthy controls.

Discussion: Our study provides new evidence for the involvement of NKG2D and its ligand ULBP4 in MS pathology. Our results point to ULBP4 as a viable target to specifically block 1 component of the NKG2D pathway without altering immune surveillance involving other NKG2DL.

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应激信号ULBP4，一种NKG2D配体，在多发性硬化症中上调并影响CD8+ t细胞行为

背景和目的:我们假设自然杀伤群2D (NKG2D)途径通过特异性NKG2D配体(nkg2dl)的存在参与多发性硬化症(MS)病理。我们的目的是评估NKG2DL在MS患者中枢神经系统和脑脊液中的表达，并鉴定诱导ul16结合蛋白4 (ULBP4)表达的细胞应激源，ul16结合蛋白4是唯一可检测到的NKG2DL。最后，我们评估了ULBP4对细胞因子产生和CD8+ T淋巴细胞运动等功能的影响，CD8+ T淋巴细胞是主要表达NKG2D的同源受体亚群。方法:采用MS患者和对照组的人死后脑组织和脑脊液检测NKG2DL的表达。利用人星形胶质细胞和神经元的原代培养进行体外实验，以鉴定诱导ULBP4表达的应激源。从MS供体和年龄/性别匹配的健康对照中分离人CD8+ T淋巴细胞，以评估可溶性ULBP4对功能的影响。结果:我们在MS患者和对照组的脑样品中检测到8种鉴定的人类nkg2dl的mRNA编码，但Western blot检测到只有ULBP4蛋白的表达。与来自MS供体的正常灰质和来自对照的白质和灰质相比，MS患者的ULBP4水平更高，特别是在活动性和慢性活动性病变和正常白质中。可溶性ULBP4也在MS患者和对照组的脑脊液中检测到，但与对照组和男性MS患者相比，女性MS患者脑脊液中较小的25 kDa的脱落/可溶性形式显著升高。我们的数据表明，可溶性ULBP4影响CD8+ T淋巴细胞的各种功能。首先，它增强了促炎细胞因子GM-CSF和干扰素-γ (ifn -γ)的产生。其次，它增加了CD8+ T淋巴细胞的运动性，并在人类星形胶质细胞存在下培养时倾向于激酶样行为。与健康对照相比，MS患者的CD8+ T淋巴细胞尤其因可溶性ULBP4的存在而改变。讨论:我们的研究为NKG2D及其配体ULBP4参与MS病理提供了新的证据。我们的研究结果表明，ULBP4是一个可行的靶点，可以特异性阻断NKG2D途径的1组分，而不会改变涉及其他NKG2DL的免疫监视。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Neurology(R) neuroimmunology & neuroinflammation

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