达沙替尼干扰HIV-1前病毒整合和HIV感染者单核细胞衍生巨噬细胞的炎症潜能。

IF 5.3 2区 医学 Q1 PHARMACOLOGY & PHARMACY Biochemical pharmacology Pub Date : 2024-09-01 DOI:10.1016/j.bcp.2024.116512
Sara Rodríguez-Mora , Clara Sánchez-Menéndez , Guiomar Bautista-Carrascosa , Elena Mateos , Lucia Moreno-Serna , Diego Megías , Juan Cantón , Valentín García-Gutiérrez , María Aránzazu Murciano-Antón , Miguel Cervero , Adam Spivak , Vicente Planelles , Mayte Coiras
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引用次数: 0

摘要

抗逆转录病毒疗法(ART)可有效控制 HIV-1 感染,但病毒在 CD4 + T 细胞和巨噬细胞形成的长效储库中的持续存在阻碍了病毒的根除,并造成了慢性炎症环境。达沙替尼是一种酪氨酸激酶抑制剂,临床上用于治疗慢性髓性白血病(CML),它也具有抗炎潜力。我们以前曾报道,达沙替尼通过保留 SAMHD1 的抗病毒活性,能非常有效地干扰 CD4 + T 细胞的 HIV-1 感染。SAMHD1 是一种先天性免疫因子,能阻止 T 细胞的活化和增殖,并通过 T592 处的磷酸化(pSAMHD1)而失活。我们观察到,用达沙替尼进行体外短期治疗可显著降低从艾滋病病毒感染者(PWH)和健康供体中分离出来的单核细胞衍生巨噬细胞(MDMs)中的pSAMHD1,从而干扰HIV-1感染。这种抑制作用基于低水平的 2-LTR 圈和前病毒整合,而病毒反转录不受影响。从长期接受达沙替尼治疗的慢性骨髓性白血病患者体内分离出的MDMs也显示出较低水平的pSAMHD1,并对HIV-1感染具有抵抗力。此外,达沙替尼通过减少M1相关细胞因子如TNFα、IL-1β、IL-6、CXCL8和CXCL9的释放,降低了MDMs的炎症潜能,但通过正常水平的IL-12和IFNγ保持了抗病毒活性。由于 IL-1RA 和 IL-10 等 M2 相关抗炎细胞因子的产生也受到影响,达沙替尼似乎干扰了 MDMs 的分化。达沙替尼与抗逆转录病毒疗法(ART)一起使用,可用于对抗CD4和巨噬细胞中的HIV-1储库,并缓解PWH特有的慢性炎症。
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Dasatinib interferes with HIV-1 proviral integration and the inflammatory potential of monocyte-derived macrophages from people with HIV

HIV-1 infection is efficiently controlled by the antiretroviral treatment (ART) but viral persistence in long-lived reservoirs formed by CD4 + T cells and macrophages impedes viral eradication and creates a chronic inflammatory environment. Dasatinib is a tyrosine kinase inhibitor clinically used against chronic myeloid leukemia (CML) that has also showed an anti-inflammatory potential. We previously reported that dasatinib is very efficient at interfering with HIV-1 infection of CD4 + T cells by preserving the antiviral activity of SAMHD1, an innate immune factor that blocks T-cell activation and proliferation and that is inactivated by phosphorylation at T592 (pSAMHD1). We observed that short-term treatment in vitro with dasatinib significantly reduced pSAMHD1 in monocyte-derived macrophages (MDMs) isolated from people with HIV (PWH) and healthy donors, interfering with HIV-1 infection. This inhibition was based on low levels of 2-LTR circles and proviral integration, while viral reverse transcription was not affected. MDMs isolated from people with CML on long-term treatment with dasatinib also showed low levels of pSAMHD1 and were resistant to HIV-1 infection. In addition, dasatinib decreased the inflammatory potential of MDMs by reducing the release of M1-related cytokines like TNFα, IL-1β, IL-6, CXCL8, and CXCL9, but preserving the antiviral activity through normal levels of IL-12 and IFNγ. Due to the production of M2-related anti-inflammatory cytokines like IL-1RA and IL-10 was also impaired, dasatinib appeared to interfere with MDMs differentiation. The use of dasatinib along with ART could be used against HIV-1 reservoir in CD4 and macrophages and to alleviate the chronic inflammation characteristic of PWH.

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来源期刊
Biochemical pharmacology
Biochemical pharmacology 医学-药学
CiteScore
10.30
自引率
1.70%
发文量
420
审稿时长
17 days
期刊介绍: Biochemical Pharmacology publishes original research findings, Commentaries and review articles related to the elucidation of cellular and tissue function(s) at the biochemical and molecular levels, the modification of cellular phenotype(s) by genetic, transcriptional/translational or drug/compound-induced modifications, as well as the pharmacodynamics and pharmacokinetics of xenobiotics and drugs, the latter including both small molecules and biologics. The journal''s target audience includes scientists engaged in the identification and study of the mechanisms of action of xenobiotics, biologics and drugs and in the drug discovery and development process. All areas of cellular biology and cellular, tissue/organ and whole animal pharmacology fall within the scope of the journal. Drug classes covered include anti-infectives, anti-inflammatory agents, chemotherapeutics, cardiovascular, endocrinological, immunological, metabolic, neurological and psychiatric drugs, as well as research on drug metabolism and kinetics. While medicinal chemistry is a topic of complimentary interest, manuscripts in this area must contain sufficient biological data to characterize pharmacologically the compounds reported. Submissions describing work focused predominately on chemical synthesis and molecular modeling will not be considered for review. While particular emphasis is placed on reporting the results of molecular and biochemical studies, research involving the use of tissue and animal models of human pathophysiology and toxicology is of interest to the extent that it helps define drug mechanisms of action, safety and efficacy.
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