Pregabalin as a Pain Therapeutic: Beyond Calcium Channels

Abstract: PHARMACOLOGY AND PROTEIN INTERACTIONS OF PREGABALIN Pregabalin Is a High-Affinity α2δ Subunit Ligand The alpha-2-delta (α2δ) subunits were first described as auxiliary subunits of the high voltageactivated calcium channels and are encoded by four genes: α2δ1, α2δ-2, α2δ-3 and α2δ-4. α2δ-1-3 are expressed in neurons as well as heart and skeletal muscle tissue (Gong et al., 2001), whereas α2δ-4 is found in non-neuronal cell types such as the retina and endocrine tissues (Dolphin, 2013). Pregabalin selectively bi… Show more

“…These features separate opioids from other common analgesic drugs that limit the production of pronociceptive mediators [for example, non-steroidal anti-inflammatory drugs (NSAIDs) (249)] or affect the function of primary afferent nociceptors (including sodium channel or calcium channel blockers such as lidocaine and ziconotide, respectively) or for which the molecular and circuit mechanisms of action remain unclear (such as gabapentinoids, anticonvulsants, and antidepressants). For example, activation of the gabapentin receptor 2-1, in addition to its effects on ion channels (250,251), can promote excitatory synaptogenesis in response to thrombospondin released by astrocytes in the SC DH (252,253). Gabapentin blocks this synaptogenesis mechanism, which may contribute to central sensitization during chronic neuropathic pain.…”

Brain circuits for pain and its treatment

“…These features separate opioids from other common analgesic drugs that limit the production of pronociceptive mediators [for example, non-steroidal anti-inflammatory drugs (NSAIDs) (249)] or affect the function of primary afferent nociceptors (including sodium channel or calcium channel blockers such as lidocaine and ziconotide, respectively) or for which the molecular and circuit mechanisms of action remain unclear (such as gabapentinoids, anticonvulsants, and antidepressants). For example, activation of the gabapentin receptor 2-1, in addition to its effects on ion channels (250,251), can promote excitatory synaptogenesis in response to thrombospondin released by astrocytes in the SC DH (252,253). Gabapentin blocks this synaptogenesis mechanism, which may contribute to central sensitization during chronic neuropathic pain.…”

Brain circuits for pain and its treatment

“…The Food and Drug Administration (FDA) has approved 3 drugs for the treatment of FM: pregabalin (PGB), duloxetine, and milnacipran (MLN) 5 . PGB, a ligand for the α2‐δ subunit of voltage‐gated calcium channels, is thought to decrease the transmission of nociceptive signals via ascending pain pathways by modulating the calcium‐dependent release of excitatory neurotransmitters such as glutamate and substance P. Hence, this drug is used to decrease pain and improve sleep 6 . Duloxetine and MLN are dual reuptake inhibitors which are proposed to increase norepinephrine and serotonin signaling in the descending pain pathways, resulting in inhibition of pain signaling in the CNS 7 .…”

Efficacy of pregabalin as a monotherapy versus combined pregabalin and milnacipran in the management of fibromyalgia

“…They are able to inhibit the influx of calcium ions into the cell and thereby modulate neurotransmission. This mechanism of action is suggested to also decrease the hyperexcitability caused by neuropathic pain, discussed in Section 6.1 (recently reviewed in Alles et al, 2020). Kopel and Browner (2020) suggest the administration of pregabalin to patients which do not respond to gabapentin treatment.…”

Neuropathic pain: Spotlighting anatomy, experimental models, mechanisms, and therapeutic aspects