TAFA4 relieves injury-induced mechanical hypersensitivity through LDL receptors and modulation of spinal A-type K+ current.

Sungjae Yoo,Andrew J Saurin,Andrew J Saurin,Andrew J Saurin,Stéphane Gaillard,Abderazzak El Khallouqi,Rafaelle Rossignol,Jean-Yves Springael,Marc Parmentier,Aziz Moqrich,Aziz Moqrich,Aziz Moqrich,Ana Reynders,Ana Reynders,Ana Reynders,Nadine Clerc,Nadine Clerc,Nadine Clerc,Francis Castets,Francis Castets,Francis Castets,Catarina Santos,Catarina Santos,Catarina Santos,Aude Charron,Aude Charron,Aude Charron,Irène Marics,Irène Marics,Irène Marics,Pascale Malapert,Pascale Malapert,Pascale Malapert,Jean-Marc Goaillard,Jean-Marc Goaillard,Sophie Ugolini,Sophie Ugolini,Sophie Ugolini,Sophie Ugolini

doi:10.1016/j.celrep.2021.109884

Abstract

Pain, whether acute or persistent, is a serious medical problem worldwide. However, its management remains unsatisfactory, and new analgesic molecules are required. We show here that TAFA4 reverses inflammatory, postoperative, and spared nerve injury (SNI)-induced mechanical hypersensitivity in male and female mice. TAFA4 requires functional low-density lipoprotein receptor-related proteins (LRPs) because their inhibition by RAP (receptor-associated protein) dose-dependently abolishes its antihypersensitive actions. SNI selectively decreases A-type K+ current (IA) in spinal lamina II outer excitatory interneurons (L-IIo ExINs) and induces a concomitant increase in IA and decrease in hyperpolarization-activated current (Ih) in lamina II inner inhibitory interneurons (L-IIi InhINs). Remarkably, SNI-induced ion current alterations in both IN subtypes were rescued by TAFA4 in an LRP-dependent manner. We provide insights into the mechanism by which TAFA4 reverses injury-induced mechanical hypersensitivity by restoring normal spinal neuron activity and highlight the considerable potential of TAFA4 as a treatment for injury-induced mechanical pain.

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