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Therapeutic Potential of Targeting TREM-1 in Inflammatory Diseases and Cancer

机译:靶向TREM-1在炎性疾病和癌症中的治疗潜力

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The triggering receptor expressed on myeloid cells (TREM)-1 is a member of the Ig-like immunoregulatory receptor family and a major amplifier of innate immune responses. TREM-1 has been implicated in the development and perpetuation of a number of inflammatory disorders, and soluble TREM-1 levels are a clinically valuable diagnostic and prognostic biomarker in patients with sepsis and other types of acute and chronic inflammation-associated diseases, easily detectable in biological fluids. High TREM-1 expression in macrophages infiltrating human tumors and increased concentrations of soluble TREM-1 also correlate with aggressive tumor behavior and recurrence and are a relevant independent predictor of poor patient survival. Pharmacological inhibition of TREM-1 has proven effective in preclinical mouse models of infectious and non-infectious inflammatory disorders and malignancies, conferring survival advantages and protecting from organ damage or tumor growth by attenuating inflammatory responses. This review aims at providing a comprehensive overview of the state of the art on TREM-1 research. We review the literature addressing TREM-1 role in the amplification of myeloid cell inflammatory responses at pathologic sites and its relevance in the development, severity, and progression of inflammatory diseases and cancer. Furthermore, we discuss recent advances in the pharmacological use of TREM-1 inhibitors in mouse preclinical models, emphasizing their potential in new strategies for the treatment of acute and chronic inflammatory conditions and for therapeutic intervention in cancer. This information will be of value to investigators in the field of pharmacology, drawing attention to novel therapeutic opportunities to complement current treatment approaches.
机译:髓样细胞(TREM)-1上表达的触发受体是Ig样免疫调节受体家族的成员,是先天免疫应答的主要扩增子。 TREM-1与多种炎性疾病的发展和永存有关,可溶性TREM-1水平是败血症和其他类型的急性和慢性炎症相关疾病患者的临床有价值的诊断和预后生物标志物,易于检测在生物液体中。在浸润人肿瘤的巨噬细胞中高TREM-1表达和可溶性TREM-1浓度升高也与侵袭性肿瘤行为和复发相关,并且是患者生存不良的独立预测因子。 TREM-1的药理学抑制作用已被证明在临床前的传染性和非传染性炎性疾病和恶性肿瘤小鼠模型中有效,赋予其生存优势,并通过减弱炎症反应来保护器官免受损伤或肿瘤生长。这篇综述旨在提供有关TREM-1研究的最新技术的全面概述。我们回顾了有关TREM-1在病理部位髓样细胞炎性反应的扩增中的作用及其与炎性疾病和癌症的发生,严重程度和进展的相关性的文献。此外,我们讨论了在小鼠临床前模型中TREM-1抑制剂在药理学用途方面的最新进展,强调了它们在治疗急性和慢性炎症以及治疗癌症的新策略中的潜力。该信息对于药理学领域的研究人员将具有重要意义,引起人们对新型治疗机会的关注,以补充当前的治疗方法。

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