van der Heide Verena, Laghlali Gabriel, Davenport Bennett, Cubitt Beatrice, Roudko Vladimir, Choo Daniel, Jhun Kevin, Humblin Etienne, Vaidya Abishek, Angeliadis Krista, Dawson Travis, Furtado Glaucia, Kamphorst Alice O, Schotsaert Michael, Ahmed Rafi, de la Torre Juan Carlos, Homann Dirk
Marc and Jennifer Lipschultz Precision Immunology Institute, Department of Immunology and Immunotherapy, Icahn School of Medicine at Mount Sinai (ISMMS), New York, NY 10029, USA.
Department of Microbiology, ISMMS, New York, NY 10029, USA; Global Health and Emerging Pathogens Institute, ISMMS, New York, NY 10029, USA; Department of Pharmaceutics, Ghent University, 9000 Ghent, Belgium.
Immunity. 2025 Jul 8;58(7):1742-1761.e14. doi: 10.1016/j.immuni.2025.05.025. Epub 2025 Jun 25.
Generation of functional memory CD8 T cells typically requires engagement of CD4 T cells. In certain acutely resolving infections, however, effector and memory CD8 T (Tmem) cell formation appears impervious to the lack of CD4 T cell help. Nevertheless, "helpless" CD8 Tmem cells may respond poorly upon rechallenge. The origin and long-term fate of helpless CD8 Tmem cells remain incompletely understood. Using multiple host-pathogen systems, we demonstrate that helpless effector CD8 T cell differentiation was largely normal, with a paradoxical accumulation of TCF1 "memory precursors." However, exposure of CD8 T cells to residual antigen impaired the development of the Tmem pool. These defects eventually resolved over time, with full restoration of memory potential and recall capacity. Our findings identify prolonged antigen presentation under helpless conditions as an essential determinant for transient CD8 Tmem cell dysfunction in acutely resolving infections and highlight plasticity within the Tmem compartment, with implications for vaccination strategies and beyond.
功能性记忆性CD8 T细胞的产生通常需要CD4 T细胞的参与。然而,在某些急性消退性感染中,效应性和记忆性CD8 T(Tmem)细胞的形成似乎不受缺乏CD4 T细胞辅助的影响。尽管如此,“无辅助”的CD8 Tmem细胞在再次受到攻击时可能反应不佳。无辅助的CD8 Tmem细胞的起源和长期命运仍未完全了解。使用多种宿主-病原体系统,我们证明无辅助的效应性CD8 T细胞分化在很大程度上是正常的,伴有TCF1“记忆前体”的反常积累。然而,CD8 T细胞暴露于残留抗原会损害Tmem库的发育。这些缺陷最终会随着时间的推移而得到解决,记忆潜能和回忆能力会完全恢复。我们的研究结果表明,在无辅助条件下延长抗原呈递是急性消退性感染中CD8 Tmem细胞短暂功能障碍的一个重要决定因素,并突出了Tmem区室的可塑性,这对疫苗接种策略及其他方面具有重要意义。