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Cited 180 time in webofscience Cited 203 time in scopus
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Attenuated pain responses in mice lacking Ca(V)3.2 T-type channels

Authors
Choi, S.Na, H. S.Kim, J.Lee, J.Lee, S.Kim, D.Park, J.Chen, C.-C.Campbell, K. P.Shin, H.-S.
Issue Date
Jul-2007
Publisher
BLACKWELL PUBLISHING
Keywords
chemical pain; mechanical pain; neuropathic pain; spinal nerve ligation ( SNL); thermal pain; tonic inflammatory pain
Citation
GENES BRAIN AND BEHAVIOR, v.6, no.5, pp 425 - 431
Pages
7
Indexed
SCIE
SCOPUS
Journal Title
GENES BRAIN AND BEHAVIOR
Volume
6
Number
5
Start Page
425
End Page
431
URI
https://scholarworks.korea.ac.kr/kumedicine/handle/2020.sw.kumedicine/35877
DOI
10.1111/j.1601-183X.2006.00268.x
ISSN
1601-1848
1601-183X
Abstract
Although T-type Ca2+ channels are implicated in nociception, the function of specific subtypes has not been well defined. Here, we compared pain susceptibility in mice lacking Ca(V)3.2 subtype of T-type Ca2+ channels (Ca(V)3.2(-/-)) with wild-type littermates in various behavioral models of pain to explore the roles of Ca(V)3.2 in the processing of noxious stimuli in vivo. In acute mechanical, thermal and chemical pain tests, Ca(V)3.2(-/-) mice showed decreased pain responses compared to wild-type mice. Ca(V)3.2(-/-) mice also displayed attenuated pain responses to tonic noxious stimuli such as intraperitoneal injections of irritant agents and intradermal injections of formalin. In spinal nerve ligation-induced neuropathic pain, however, behavioral responses of Ca(V)3.2(-/-) mice were not different from those of wild-type mice. The present study reveals that the Ca(V)3.2 subtype of T-type Ca2+ channels are important in the peripheral processing of noxious signals, regardless of modality, duration or affected tissue type.
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