Kirin Gada scite author profile

Chronic pain is a debilitating and increasingly common medical problem with few effective treatments. In addition to the direct and indirect economic burden of pain syndromes, the concomitant increase in prescriptions for narcotics has contributed to a sharp rise in deaths associated with drug misuse – the ‘opioid crisis’. Together, these issues highlight the unmet clinical and social need for a new generation of safe, efficacious analgesics. The detection and transmission of pain stimuli is largely mediated by somatosensory afferent fibres of the dorsal root ganglia. These nociceptive cells express an array of membrane proteins that have received significant attention as attractive targets for new pain medications. Among these, a growing body of evidence supports a role for the two‐pore domain potassium (K2P) family of K+ channels. Here, we provide a concise review of the K2P channels, their role in pain biology and their potential as targets for novel analgesic agents.

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PKC regulation of ion channels: The involvement of PIP2

Gada

Logothetis

2022

Journal of Biological Chemistry

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A novel small-molecule selective activator of homomeric GIRK4 channels

Cui

Gada

et al. 2022

Journal of Biological Chemistry

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An optogenetic tool to recruit individual PKC isozymes to the cell surface and promote specific phosphorylation of membrane proteins

Gada

Kawano

Plant

et al. 2022

Journal of Biological Chemistry

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Hypoxia inhibits the cardiac I current through SUMO targeting Kir2.1 activation by PIP2

Xu¹,

Yang²,

Chandrashekar³

et al. 2022

iScience

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Kirin Gada

Two‐pore domain potassium channels: emerging targets for novel analgesic drugs: IUPHAR Review 26

PKC regulation of ion channels: The involvement of PIP2

A novel small-molecule selective activator of homomeric GIRK4 channels

An optogenetic tool to recruit individual PKC isozymes to the cell surface and promote specific phosphorylation of membrane proteins

Hypoxia inhibits the cardiac I current through SUMO targeting Kir2.1 activation by PIP2

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