TEX264

Last update 08 May 2025

Basic Info

Synonyms

FLJ13935, Putative secreted protein Zsig11, testis expressed 264, ER-phagy receptor

+ [3]

Introduction

Major reticulophagy (also called ER-phagy) receptor that acts independently of other candidate reticulophagy receptors to remodel subdomains of the endoplasmic reticulum into autophagosomes upon nutrient stress, which then fuse with lysosomes for endoplasmic reticulum turnover (PubMed:31006537, PubMed:31006538). The ATG8-containing isolation membrane (IM) cradles a tubular segment of TEX264-positive ER near a three-way junction, allowing the formation of a synapse of 2 juxtaposed membranes with trans interaction between the TEX264 and ATG8 proteins (PubMed:31006537). Expansion of the IM would extend the capture of ER, possibly through a 'zipper-like' process involving continued trans TEX264-ATG8 interactions, until poorly understood mechanisms lead to the fission of relevant membranes and, ultimately, autophagosomal membrane closure (PubMed:31006537). Also involved in the repair of covalent DNA-protein cross-links (DPCs) during DNA synthesis: acts by bridging VCP/p97 to covalent DNA-protein cross-links (DPCs) and initiating resolution of DPCs by SPRTN (PubMed:32152270).

100 Clinical Results associated with TEX264

100 Translational Medicine associated with TEX264

0 Patents (Medical) associated with TEX264

Literatures (Medical) associated with TEX264

04 Mar 2025·Autophagy

Autophagy as a way to remove DNA lesions

Article

Author: Lei, Yuchen ; Klionsky, Daniel J.

Type I topoisomerases (TOP1) are critical to remove the topological stress when DNA double strands are unwound. The TOP1 cleavage complexes (TOP1cc) are normally transient, and the stabilization of TOP1cc by its inhibitors, such as camptothecin (CPT), may lead to DNA damage and become cytotoxic. The proteasome pathway degrades trapped TOP1, which is necessary for the repair machinery to gain access to the DNA; however, this process is mainly described when the CPT concentration is high, at levels which are clinically unachievable. In a recently published study, Lascaux et al. identify macroautophagy/autophagy as a new pathway to remove DNA lesions upon clinically relevant low-dose CPT treatment. The autophagy receptor TEX264 binds to TOP1 and brings this protein and its bound DNA fragments to the phagophore; subsequently, they are ultimately delivered to the lysosome for degradation. This study demonstrates the role of autophagy in maintaining genome stability from a new perspective and reveals potential targets to deal with the resistance to TOP1cc inhibitors during cancer treatment.

01 Jan 2025·Trends in Biochemical Sciences

TEX264-mediated selective autophagy directs DNA damage repair

Article

Author: Suzuki, Sho W ; Qi, Yuxia

DNA is constantly subject to damage from endogenous and exogenous factors, leading to mutations and disease. While DNA is traditionally repaired in the nucleus, Lascaux et al. reveal a novel role for the lysosome in DNA repair, demonstrating that topoisomerase 1 (TOP1) cleavage complex (TOP1cc) DNA lesions are degraded via TEX264-mediated selective autophagy.

01 Oct 2024·Cell

TEX264 drives selective autophagy of DNA lesions to promote DNA repair and cell survival

Article

Author: Torrecilla, Ignacio ; Koukouravas, Stelios ; Trugenberger, Camilla ; Maughan, Tim ; Otten, Cecile ; Vendrell, Iolanda ; Popović, Marta ; Yang, Hongbin ; Song, Wei ; Ruggiano, Annamaria ; Carrique, Loïc ; Domingo, Enric ; Tribble, Sara ; Fischer, Roman ; Ngeow, Joanne ; Milošević, Ira ; Ng, Alvin Wei Tian ; Bancroft, James ; Lascaux, Pauline ; Antičević, Ivan ; D’Angiolella, Vincenzo ; Peron, Cristiano ; Aljarbou, Ftoon ; Johnson, Errin ; Raimundo, Nuno ; Hoslett, Gwendoline ; Deangeli, Giulio ; Ramadan, Kristijan ; Zhao, Yichen ; D'Angiolella, Vincenzo

DNA repair and autophagy are distinct biological processes vital for cell survival. Although autophagy helps maintain genome stability, there is no evidence of its direct role in the repair of DNA lesions. We discovered that lysosomes process topoisomerase 1 cleavage complexes (TOP1cc) DNA lesions in vertebrates. Selective degradation of TOP1cc by autophagy directs DNA damage repair and cell survival at clinically relevant doses of topoisomerase 1 inhibitors. TOP1cc are exported from the nucleus to lysosomes through a transient alteration of the nuclear envelope and independent of the proteasome. Mechanistically, the autophagy receptor TEX264 acts as a TOP1cc sensor at DNA replication forks, triggering TOP1cc processing by the p97 ATPase and mediating the delivery of TOP1cc to lysosomes in an MRE11-nuclease- and ATR-kinase-dependent manner. We found an evolutionarily conserved role for selective autophagy in DNA repair that enables cell survival, protects genome stability, and is clinically relevant for colorectal cancer patients.

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TEX264

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