化学
配体(生物化学)
生物物理学
离解率
分子
离解(化学)
受体
生物化学
生物
物理化学
有机化学
作者
Kaitao Li,Paul Cárdenas-Lizana,Jintian Lyu,Anna Kellner,Menglan Li,Peiwen Cong,Valencia Watson,Zhou Yuan,Eunseon Ahn,Larissa Doudy,Zhenhai Li,Khalid Salaita,Rafi Ahmed,Cheng Zhu
标识
DOI:10.1038/s41467-024-52565-2
摘要
Despite the success of PD-1 blockade in cancer therapy, how PD-1 initiates signaling remains unclear. Soluble PD-L1 is found in patient sera and can bind PD-1 but fails to suppress T cell function. Here, we show that PD-1 function is reduced when mechanical support on ligand is removed. Mechanistically, cells exert forces to PD-1 and prolong bond lifetime at forces <7 pN (catch bond) while accelerate dissociation at forces >8pN (slip bond). Molecular dynamics of PD-1-PD-L2 complex suggests force may cause relative rotation and translation between the two molecules yielding distinct atomic contacts not observed in the crystal structure. Compared to wild-type, PD-1 mutants targeting the force-induced distinct interactions maintain the same binding affinity but suppressed/eliminated catch bond, lowered rupture force, and reduced inhibitory function. Our results uncover a mechanism for cells to probe the mechanical support of PD-1-PD-Ligand bonds using endogenous forces to regulate PD-1 signaling.
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