IL-11—An aging-related cytokine with opportunities for regulating hematopoiesis

IF 7.6 2区 医学 Q1 HEMATOLOGY
HemaSphere Pub Date : 2024-11-19 DOI:10.1002/hem3.70050
David G. Kent
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Studying them at scale in a tissue context has been challenging due to functional redundancy and pleiotropic effects, but they remain an area of active investigation for a wide range of groups, especially now that new approaches are emerging to studying cytokine signaling dynamics at the single molecule level.<span><sup>1-3</sup></span> This summer, a huge study on the proinflammatory cytokine Interleukin 11 (IL-11) emerged in <i>Nature</i> magazine from the group of Stuart Cook—the paper <i>Inhibition of IL-11 signaling extends mammalian healthspan and lifespan</i><span><sup>4</sup></span> dropped into the hyperactive aging research community and caused quite a stir.</p><p>The headline statement: “Genetic deletion of <i>Il11</i> extended the lives of mice of both sexes, by 24.9% on average” caught the research world's attention. This was impressively followed by a series of studies that involved treating mice with an anti-IL-11 antibody from middle age (75 weeks) until death where the researchers observed another impressive increase in lifespan (&gt;20%), strongly suggesting that early life events do not irrevocably sentence an organism to an early death. Simple in design and elegant in execution, the study details the genetic and pharmacological modulation of aging in both sexes. This positions the paper as one of the few that demonstrates a clear extension of lifespan through the removal of a single gene—one of the earliest examples of which is the <i>daf-2</i> c.elegans mutants<span><sup>5</sup></span> that have an extended lifespan. The authors go on to detail a wide range of metabolic and pathway profiling and imply that the metabolic, proinflammatory, and profibrotic roles of IL-11 are the mechanistic drivers of aging through the ERK-mTORC1 and JAK/STAT signaling pathways. This also suggests that JAK inhibitors, metformin, rapamycin, and so forth might have antiaging and antifibrotic roles as well, but the authors note that some of these current therapies struggle with on- and off-target toxicities that an anti-IL-11 therapy might not have. Indeed, an early-stage clinical trial is already underway using anti-IL-11 for the treatment of fibro-inflammatory diseases.</p><p>IL-11 is no stranger to stem cell and hematopoiesis research. It is one of a handful of critical molecules that interact with the glycoprotein 130 (gp130) family for signal transduction, in the good company of leukemia inhibitory factor (LIF) and interleukin 6 (IL-6) among others. These molecules have long been studied in stem cell systems (e.g., LIF in mouse embryonic stem cells and ciliary neurotrophic factor [CNTF] in neural stem cells) and have also been among the key regulators of hematopoietic stem cell (HSC) self-renewal in the form of IL-6 and IL-11. Early studies highlighted IL-11's partnership with the stem cell factor (SCF) in maintaining self-renewal in HSC expansion cultures,<span><sup>6, 7</sup></span> but equally, IL-11 has been shown to be dispensable for the more recent and better performing PVA-based cultures systems described by Yamazaki and colleagues which used thrombopoietin (TPO) and SCF to achieve HSC expansion.<span><sup>8</sup></span> Interestingly, however, IL-11 on its own has been recently shown to maintain HSCs in a hibernating state outside the body in both the mouse and human settings.<span><sup>9, 10</sup></span> HSCs were maintained as single cells in the absence of a physical niche and retained their full functional potential in transplantation assays compared to freshly isolated HSCs. 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引用次数: 0

Abstract

Cytokines have long been known as chemical messengers that act upon cells in the blood system to induce proliferation and response to disease. Studying them at scale in a tissue context has been challenging due to functional redundancy and pleiotropic effects, but they remain an area of active investigation for a wide range of groups, especially now that new approaches are emerging to studying cytokine signaling dynamics at the single molecule level.1-3 This summer, a huge study on the proinflammatory cytokine Interleukin 11 (IL-11) emerged in Nature magazine from the group of Stuart Cook—the paper Inhibition of IL-11 signaling extends mammalian healthspan and lifespan4 dropped into the hyperactive aging research community and caused quite a stir.

The headline statement: “Genetic deletion of Il11 extended the lives of mice of both sexes, by 24.9% on average” caught the research world's attention. This was impressively followed by a series of studies that involved treating mice with an anti-IL-11 antibody from middle age (75 weeks) until death where the researchers observed another impressive increase in lifespan (>20%), strongly suggesting that early life events do not irrevocably sentence an organism to an early death. Simple in design and elegant in execution, the study details the genetic and pharmacological modulation of aging in both sexes. This positions the paper as one of the few that demonstrates a clear extension of lifespan through the removal of a single gene—one of the earliest examples of which is the daf-2 c.elegans mutants5 that have an extended lifespan. The authors go on to detail a wide range of metabolic and pathway profiling and imply that the metabolic, proinflammatory, and profibrotic roles of IL-11 are the mechanistic drivers of aging through the ERK-mTORC1 and JAK/STAT signaling pathways. This also suggests that JAK inhibitors, metformin, rapamycin, and so forth might have antiaging and antifibrotic roles as well, but the authors note that some of these current therapies struggle with on- and off-target toxicities that an anti-IL-11 therapy might not have. Indeed, an early-stage clinical trial is already underway using anti-IL-11 for the treatment of fibro-inflammatory diseases.

IL-11 is no stranger to stem cell and hematopoiesis research. It is one of a handful of critical molecules that interact with the glycoprotein 130 (gp130) family for signal transduction, in the good company of leukemia inhibitory factor (LIF) and interleukin 6 (IL-6) among others. These molecules have long been studied in stem cell systems (e.g., LIF in mouse embryonic stem cells and ciliary neurotrophic factor [CNTF] in neural stem cells) and have also been among the key regulators of hematopoietic stem cell (HSC) self-renewal in the form of IL-6 and IL-11. Early studies highlighted IL-11's partnership with the stem cell factor (SCF) in maintaining self-renewal in HSC expansion cultures,6, 7 but equally, IL-11 has been shown to be dispensable for the more recent and better performing PVA-based cultures systems described by Yamazaki and colleagues which used thrombopoietin (TPO) and SCF to achieve HSC expansion.8 Interestingly, however, IL-11 on its own has been recently shown to maintain HSCs in a hibernating state outside the body in both the mouse and human settings.9, 10 HSCs were maintained as single cells in the absence of a physical niche and retained their full functional potential in transplantation assays compared to freshly isolated HSCs. Taken in the context of the new findings from the Cook group, it now becomes critical to work out the relationship of IL-11 signaling in aging HSCs—what would be blocking this key regulator during HSC aging and how would it influence the acquisition of clonal hematopoiesis, accumulation of inflammatory cytokines, or leukemia development? Perhaps, one of the most interesting areas to consider is that the hibernation cultures are fully reversible with respect to HSC function whereas the Cook study draws the linkage to IL-11 driving an irreversible senescent state.

In any event, it almost seems certain that the anti-IL-11 therapy described in the paper will be explored widely for its potential application in humans. It will be incredibly interesting to understand the changes in the blood system, and more specifically on HSCs and inflammation-induced changes with aging. A 25% extended lifespan from blocking a single molecule seems too good to be true from a direct translation to the human point of view, but every little bit helps and there is almost certainly some fascinating science to unearth.

David G. Kent is the sole author and wrote the article.

The author declares no conflict of interest.

The Kent lab is funded by the UK Medical Research Council, the Bill and Melinda Gates Foundation, Blood Cancer UK, the Rosetrees Trust, and Cancer Research UK.

IL-11--一种与衰老有关的细胞因子,可调节造血功能。
众所周知,细胞因子是作用于血液系统细胞的化学信使,可诱导细胞增殖并对疾病做出反应。由于功能冗余和多效应,在组织背景下大规模研究细胞因子具有挑战性,但它们仍然是众多研究小组积极研究的领域,尤其是现在出现了在单分子水平研究细胞因子信号动态的新方法。今年夏天,斯图尔特-库克(Stuart Cook)小组在《自然》杂志上发表了一篇关于促炎细胞因子白细胞介素 11(IL-11)的重要研究论文--《抑制 IL-11 信号传导可延长哺乳动物的健康寿命》(Inhibition of IL-11 signaling extends mammalian healthspan and lifespan4),这篇论文一经发表,就在亢奋的衰老研究界引起了不小的轰动:"Il11基因缺失可延长雌雄小鼠的寿命,平均延长24.9%"的标题引起了研究界的关注。随后进行的一系列研究令人印象深刻,这些研究涉及用抗IL-11抗体治疗中年(75周)至死亡的小鼠,在这些研究中,研究人员观察到小鼠的寿命再次显著延长(20%),这有力地表明,生命早期的事件并不会不可逆转地判处生物体早死。该研究设计简单,执行优雅,详细介绍了基因和药物对两性衰老的调节作用。这使这篇论文成为少数几篇通过移除单个基因明确延长寿命的论文之一--其中最早的例子是daf-2 c.elegans突变体5,它们的寿命得到了延长。作者接着详细介绍了一系列代谢和通路分析,并暗示 IL-11 的代谢、促炎和促坏死作用是通过 ERK-mTORC1 和 JAK/STAT 信号通路导致衰老的机理驱动因素。这也表明,JAK 抑制剂、二甲双胍、雷帕霉素等也可能具有抗衰老和抗纤维化的作用,但作者指出,目前的一些疗法存在靶上和脱靶毒性,而抗 IL-11 疗法可能没有这些毒性。事实上,利用抗IL-11治疗纤维炎症性疾病的早期临床试验已经在进行中。IL-11对干细胞和造血研究来说并不陌生。它是与糖蛋白130(gp130)家族相互作用进行信号转导的少数关键分子之一,与白血病抑制因子(LIF)和白细胞介素6(IL-6)等分子齐名。长期以来,人们一直在干细胞系统中研究这些分子(如小鼠胚胎干细胞中的LIF和神经干细胞中的睫状神经营养因子[CNTF]),IL-6和IL-11也是造血干细胞自我更新的关键调节因子之一。早期的研究强调了IL-11与干细胞因子(SCF)在维持造血干细胞扩增培养物自我更新方面的合作关系,6, 7 但同样,IL-11也被证明对Yamazaki及其同事所描述的最新的、性能更好的基于PVA的培养系统来说是不可或缺的,该系统使用血小板生成素(TPO)和SCF来实现造血干细胞扩增。然而,有趣的是,最近有研究表明,在小鼠和人体环境中,IL-11 本身可使造血干细胞在体外保持冬眠状态9,10 造血干细胞在没有物理龛位的情况下保持单细胞状态,与新鲜分离的造血干细胞相比,造血干细胞在移植试验中保持了全部功能潜能。从库克研究小组的新发现来看,现在研究 IL-11 信号在衰老造血干细胞中的关系变得至关重要--在造血干细胞衰老过程中,是什么阻断了这一关键调节因子,它又将如何影响克隆造血的获得、炎症细胞因子的积累或白血病的发展?也许,最值得考虑的一个方面是,冬眠培养的造血干细胞功能是完全可逆的,而库克的研究则将 IL-11 与不可逆转的衰老状态联系起来。了解血液系统的变化,更具体地说是造血干细胞的变化以及炎症引起的衰老变化,将是一件非常有趣的事情。从直接应用于人类的角度看,阻断单一分子可延长25%的寿命似乎好得不像真的,但每一点都有帮助,而且几乎肯定会有一些引人入胜的科学发现。
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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来源期刊
HemaSphere
HemaSphere Medicine-Hematology
CiteScore
6.10
自引率
4.50%
发文量
2776
审稿时长
7 weeks
期刊介绍: HemaSphere, as a publication, is dedicated to disseminating the outcomes of profoundly pertinent basic, translational, and clinical research endeavors within the field of hematology. The journal actively seeks robust studies that unveil novel discoveries with significant ramifications for hematology. In addition to original research, HemaSphere features review articles and guideline articles that furnish lucid synopses and discussions of emerging developments, along with recommendations for patient care. Positioned as the foremost resource in hematology, HemaSphere augments its offerings with specialized sections like HemaTopics and HemaPolicy. These segments engender insightful dialogues covering a spectrum of hematology-related topics, including digestible summaries of pivotal articles, updates on new therapies, deliberations on European policy matters, and other noteworthy news items within the field. Steering the course of HemaSphere are Editor in Chief Jan Cools and Deputy Editor in Chief Claire Harrison, alongside the guidance of an esteemed Editorial Board comprising international luminaries in both research and clinical realms, each representing diverse areas of hematologic expertise.
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