从血液恶性肿瘤到衰老相关疾病的 CAR T 疗法:一个不断扩大的世界。

IF 4.4 3区 医学 Q1 MEDICINE, GENERAL & INTERNAL
Davide Ramoni, Fabrizio Montecucco, Federico Carbone
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引用次数: 0

摘要

背景:基因编辑历时二十年,时间虽短但影响深远,为血液恶性肿瘤的治疗带来了重大突破。然而,尽管嵌合抗原受体 T(CAR T)已经发展了几代,但这种成功的疗法尚未在实体瘤和非肿瘤性疾病中推广:这篇叙述性综述讨论了CAR T疗法在克服实体瘤微环境的复杂性方面仍然面临的挑战,以及其长期活性在非肿瘤疾病中可能产生的未知和不可预测后果所引发的担忧:在最近的研究中,CAR T 的衰老潜能正成为一个令人兴奋的研究领域。尽管如此,实验性但有希望的结果确实表明,清除衰老细胞是改善生理衰老过程中运动能力和代谢功能障碍的有效策略,具有长期治疗和预防作用。然而,要有效扩增 CAR T 群体,需要在输注前进行淋巴清除化疗。虽然这一程序对于肿瘤疾病的抢救治疗听起来很合理,但它会带来基因毒性风险,对于非恶性疾病可能并不合理。这些是在非肿瘤性疾病中应用 CAR T 疗法的主要差距:结论:目前正在对其他类别的 CAR 细胞进行研究,我们期待着更多的研究成果。对 NK 细胞和巨噬细胞进行工程化是提高细胞毒性和免疫调节特性的候选方法,有可能扩大在实体瘤和非肿瘤性疾病中的应用。最后,对老年个体的自体 T 细胞进行工程改造可能会产生生物退化的 CAR T 克隆,其功能受损,对细胞因子释放的影响难以预测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

CAR T therapy from haematological malignancies to aging-related diseases: An ever-expanding universe

CAR T therapy from haematological malignancies to aging-related diseases: An ever-expanding universe

CAR T therapy from haematological malignancies to aging-related diseases: An ever-expanding universe

Background

Short but impactful, the two-decade story of gene editing allowed a significant breakthrough in the treatment of haematological malignancies. However, despite different generations of chimeric antigen receptor T (CAR T), such a successful therapy has not yet been replicated in solid tumours and non-oncological diseases.

Methods

This narrative review discusses how CAR T therapy still faces challenges in overcoming the complexity of the solid tumour microenvironment and the concerns that its long-term activity raises about potential unknown and unpredictable consequences in non-oncological diseases.

Results

In the most recent studies, the senolytic potential of CAR T is becoming an exciting field of research. Still, experimental but promising results indeed indicate the clearance of senescent cells as an effective strategy to improve exercise capacity and metabolic dysfunction in physiological ageing, with long-term therapeutic and preventive effects. However, an effective expansion of a CAR T population requires a lympho-depleting chemotherapy prior to infusion. While this procedure sounds reasonable for rescue therapy of oncological diseases, it poses genotoxic risks that may not be justified for non-malignant diseases. Those represent the leading gaps for applying CAR T therapy in non-oncological diseases.

Conclusion

More is expected from current studies on the other classes of CAR cells now under investigation. Engineering NK cells and macrophages are candidates to improve cytotoxic and immunomodulating properties, potentially able to broaden application in solid tumours and non-oncological diseases. Finally, engineering autologous T cells in old individuals may generate biologically deteriorated CAR T clones with impaired function and unpredictable effects on cytokine release.

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来源期刊
CiteScore
9.50
自引率
3.60%
发文量
192
审稿时长
1 months
期刊介绍: EJCI considers any original contribution from the most sophisticated basic molecular sciences to applied clinical and translational research and evidence-based medicine across a broad range of subspecialties. The EJCI publishes reports of high-quality research that pertain to the genetic, molecular, cellular, or physiological basis of human biology and disease, as well as research that addresses prevalence, diagnosis, course, treatment, and prevention of disease. We are primarily interested in studies directly pertinent to humans, but submission of robust in vitro and animal work is also encouraged. Interdisciplinary work and research using innovative methods and combinations of laboratory, clinical, and epidemiological methodologies and techniques is of great interest to the journal. Several categories of manuscripts (for detailed description see below) are considered: editorials, original articles (also including randomized clinical trials, systematic reviews and meta-analyses), reviews (narrative reviews), opinion articles (including debates, perspectives and commentaries); and letters to the Editor.
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