J Clin Invest. 2024 Mar 1;134(5):e178570. doi: 10.1172/JCI178570.
Immune tolerance to allogenic transplanted tissues remains elusive, and therapeutics promoting CD4+FOXP3+ Tregs are required to achieve this ultimate goal. In this issue of the JCI, Efe and colleagues engineered an Fc domain fused to a human mutein IL-2 (mIL-2-Fc) bearing mutations that confer preferential binding to the high-affinity IL-2 receptor expressed on Tregs. In vivo mIL-2-Fc therapy effectively heightened mouse, monkey, and human Treg numbers, promoted tolerance to minor antigen mismatched skin grafts in mice, and synergized with immunosuppressive drugs used in the clinic. These findings warrant clinical trials that assess the efficacy of mIL-2-Fc in transplantation.
异体移植组织的免疫耐受仍然难以实现,需要治疗方法来促进 CD4+FOXP3+Tregs 的产生,以实现这一最终目标。在本期 JCI 中,Efe 和同事构建了一种与人 IL-2 突变体(mIL-2-Fc)融合的 Fc 结构域,该突变体赋予了对 Tregs 上表达的高亲和力 IL-2 受体的优先结合。体内 mIL-2-Fc 治疗可有效提高小鼠、猴子和人类 Treg 数量,促进小鼠对次要抗原不匹配皮肤移植物的耐受,并与临床中使用的免疫抑制药物协同作用。这些发现值得进行临床试验,以评估 mIL-2-Fc 在移植中的疗效。
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