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  4. Expanding the Toolbox: Novel Modulators of Endolysosomal Cation Channels
 
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Expanding the Toolbox: Novel Modulators of Endolysosomal Cation Channels

Journal
Handbook of experimental pharmacology
Date Issued
2022-07-29
Author(s)
Rautenberg, Susanne
Keller, Marco
Leser, Charlotte
CHENG-CHANG CHEN  
Bracher, Franz
Grimm, Christian
DOI
10.1007/164_2022_605
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/617279
Abstract
Functional characterization of endolysosomal ion channels is challenging due to their intracellular location. With recent advances in endolysosomal patch clamp technology, it has become possible to directly measure ion channel currents across endolysosomal membranes. Members of the transient receptor potential (TRP) cation channel family, namely the endolysosomal TRPML channels (TRPML1-3), also called mucolipins, as well as the distantly related two-pore channels (TPCs) have recently been characterized in more detail with endolysosomal patch clamp techniques. However, answers to many physiological questions require work in intact cells or animal models. One major obstacle thereby is that the known endogenous ligands of TRPMLs and TPCs are anionic in nature and thus impermeable for cell membranes. Microinjection, on the other hand, is technically demanding. There is also a risk of losing essential co-factors for channel activation or inhibition in isolated preparations. Therefore, lipophilic, membrane-permeable small-molecule activators and inhibitors for TRPMLs and TPCs are urgently needed. Here, we describe and discuss the currently available small-molecule modulators of TRPMLs and TPCs.
Subjects
Lysosome; Small-molecule activator; Small-molecule inhibitor; TPC; TRPML
Type
journal article

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