Exploring protein-protein interactions for the development of new analgesics

被引:0
|
作者
do Nascimento, Alexandre Martins [1 ,2 ]
Marques, Rauni Borges [1 ,3 ]
Roldao, Allan Pradelli [1 ]
Rodrigues, Ana Maria [1 ]
Eslava, Rodrigo Mendes [1 ]
Dale, Camila Squarzoni [2 ]
Reis, Eduardo Moraes [1 ]
Schechtman, Deborah [1 ]
机构
[1] Univ Sao Paulo, Chem Inst, Dept Biochem, BR-05508000 Sao Paulo, SP, Brazil
[2] Univ Sao Paulo, Inst Biomed Sci, Dept Anat, Lab Neuromodulat Expt Pain LaNed, BR-05508000 Sao Paulo, SP, Brazil
[3] Univ Sao Paulo, Interunit Grad Program Bioinformat, BR-05508000 Sao Paulo, SP, Brazil
基金
巴西圣保罗研究基金会;
关键词
SMALL-MOLECULE INHIBITORS; PHOSPHOLIPASE-C-GAMMA; CRMP2 PEPTIDE APTAMER; NEUROPATHIC PAIN; PERIPHERAL NEUROPATHY; THERMAL HYPERALGESIA; INFLAMMATORY PAIN; NMDA RECEPTORS; NITRIC-OXIDE; PDZ DOMAIN;
D O I
10.1126/scisignal.adn4694
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The development of new analgesics has been challenging. Candidate drugs often have limited clinical utility due to side effects that arise because many drug targets are involved in signaling pathways other than pain transduction. Here, we explored the potential of targeting protein-protein interactions (PPIs) that mediate pain signaling as an approach to developing drugs to treat chronic pain. We reviewed the approaches used to identify small molecules and peptide modulators of PPIs and their ability to decrease pain-like behaviors in rodent animal models. We analyzed data from rodent and human sensory nerve tissues to build associated signaling networks and assessed both validated and potential interactions and the structures of the interacting domains that could inform the design of synthetic peptides and small molecules. This resource identifies PPIs that could be explored for the development of new analgesics, particularly between scaffolding proteins and receptors for various growth factors and neurotransmitters, as well as ion channels and other enzymes. Targeting the adaptor function of CBL by blocking interactions between its proline-rich carboxyl-terminal domain and its SH3-domain-containing protein partners, such as GRB2, could disrupt endosomal signaling induced by pain-associated growth factors. This approach would leave intact its E3-ligase functions, which are mediated by other domains and are critical for other cellular functions. This potential of PPI modulators to be more selective may mitigate side effects and improve the clinical management of pain.
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页数:15
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