Pharmacology of Cav1 (L-Type) Channels

Triggle, David J.

doi:10.1007/978-1-4419-9254-3_2

Cited by 10 publications

(11 citation statements)

References 296 publications

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“…Indeed, the firstgeneration Ca 21 channel blockers were essentially "accidental" discoveries (although it is clear, however, that these drugs have proved subsequently to be invaluable molecular tools with which to dissect and analyze channel function). 1,5,14,15,169,171,172,179 Second, the drugs were discovered in biological assay systems with a direct and readily observable relationship between the measured response in vitro and in vivo-vascular smooth muscle tension and blood pressure-and the desired therapeutic goal of antianginal and antihypertensive activity. Third, the cardiovascular system is dominated by the activity of the Ca V l class of channel; hence, differential functional contributions by other classes of channel are relatively unimportant, and fine-tuning of drug action occurs essentially within one channel class.…”

Section: Discussionmentioning

confidence: 99%

“…However, the L-type Ca 21 channel is also recognized by a wide variety of other chemical structures both naturally occurring and synthetic, consistent with a general role for ion channels as multiple pharmacological receptors. 4,5,12 Voltage-gated Ca 21 channels are members of a superfamily of ion channels that includes Na 1 , K 1 , and Ca 21 channels that share significant structural and functional homology. 13 There are several members of the Ca 21 channel subfamily that may be distinguished by their structure, subunit composition, location, function, and pharmacology ( Fig.…”

Section: Voltage-gated Calcium Channelsmentioning

confidence: 99%

“…However, the control of Ca 21 mobilization and storage processes still represents an ongoing therapeutic possibility in a variety of cardiovascular, endocrine, and neuronal disorders. [1][2][3][4][5] The physiologic control of Ca 21 depends upon a specific set of cellular conditions:…”

Section: Introductionmentioning

confidence: 99%

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Drug Targets in the Voltage-Gated Calcium Channel Family: Why Some Are and Some Are Not

Triggle

2003

ASSAY and Drug Development Technologies

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The L-type calcium channel antagonists have been, and continue to be, a very successful group of therapeutic agents targeted at cardiovascular disorders, notably angina and hypertension. The discovery that the voltage-gated calcium channels are a large and widely distributed family with important roles in both the peripheral and central nervous systems has initiated a major search for drugs active at other calcium channel types directed at disorders of the central nervous system, including pain, epilepsy, and stroke. These efforts have not been therapeutically successful thus far, and small molecule equivalents of the L-type blockers nifedipine, diltiazem, and verapamil directed at non-L-type channels have not been found. The underlying reasons for this are discussed together with suggestions for new directions, including fertility control, oxygen-sensitive channels, and calcium channel activators.

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Section: Discussionmentioning

confidence: 99%

Section: Voltage-gated Calcium Channelsmentioning

confidence: 99%

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Drug Targets in the Voltage-Gated Calcium Channel Family: Why Some Are and Some Are Not

Triggle

2003

ASSAY and Drug Development Technologies

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“…However, DHPs do not appear to discriminate among various Ca v 3 family members, and many examples in the literature showing DHP block of Ca v 3 currents [128,129,130,131] may be due to action on multiple Ca v 3 channel isoforms. In general, as demonstrated for Ca v 1 family members, DHPs interact with the domains III and IV S5-S6 regions [reviewed in 31,124, also see the review article by D. Triggle in this issue], as summarized in Fig. (1).…”

Section: Dihydropyridinesmentioning

confidence: 96%

Molecular Pharmacology of Non-L-type Calcium Channels

Doering

Zamponi²

2005

CPD

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Voltage-gated calcium channels are key sources of calcium entry into the cytosol. Mutations in calcium channels have been implicated in numerous disorders such as migraine, incomplete congenital X-linked stationary night blindness, epilepsy, and ataxia, and they are important therapeutic targets for the treatment of pain, stroke, hypertension, and epilepsy. Calcium channel antagonists can be broadly classified into three groups. 1) Inorganic ions typically nonselectively block the pore of most calcium channel subtypes, and in some cases, alter gating kinetics. 2) Peptides isolated from arachnids, cone snails, and snakes frequently selectively antagonize individual calcium channel subtypes by direct occlusion of the pore or altering gating kinetics. 3) Small organic molecules of various structure-activity-relationship (SAR) classes can mediate both selective and nonselective effects on individual calcium channel subtypes, and occlude the pore or reduce channel availability. Here, we provide an overview of classes of inhibitors of non-L-type calcium channels.

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“…The aim of our study was to describe the characteristics of four newly synthesized previously uncharacterized Biginelli type dihydropyrimidines, whose molecular conformation is in accordance with the Triggle dihydropyridine receptor binding model, [22] and to obtain novel pharmacological data regarding their activity and selectivity of action on depolarization versus noradrenaline‐induced vascular smooth muscle contraction in comparison with the reference calcium channel blocker nifedipine. Data we obtained on these novel compounds show that some exhibit a similar efficacy to that of the reference drug, with an even better selectivity for the inhibition of depolarization‐induced contraction.…”

Section: Introductionmentioning

confidence: 99%