Abstract
Intracellular calcium plays a crucial role in modulating a variety of functions such as muscle contraction, hormone secretion, gene expression, or cell growth. Calcium signaling has been however shown to be more complex than initially thought. Indeed, it is confined within cell microdomains, and different calcium channels are associated with different functions, as shown by various channelopathies. Sporadic mutations on voltage-operated L-type calcium channels in adrenal glomerulosa cells have been shown recently to be the second most prevalent genetic abnormalities present in human aldosterone-producing adenoma. The observed modification of the threshold of activation of the mutated channels not only provides an explanation for this gain of function but also reminds us on the importance of maintaining adequate electrophysiological characteristics to make channels able to exert specific cellular functions. Indeed, the contribution to steroid production of the various calcium channels expressed in adrenocortical cells is not equal, and the reason has been investigated for a long time. Given the very negative resting potential of these cells, and the small membrane depolarization induced by their physiological agonists, low threshold T-type calcium channels are particularly well suited for responding under these conditions and conveying calcium into the cell, at the right place for controlling steroidogenesis. In contrast, high threshold L-type channels are normally activated by much stronger cell depolarizations. The fact that dihydropyridine calcium antagonists, specific for L-type channels, are poorly efficient for reducing aldosterone secretion either in vivo or in vitro, strongly supports the view that these two types of channels differently affect steroid biosynthesis. Whether a similar analysis is transposable to fasciculata cells and cortisol secretion is one of the questions addressed in the present review. No similar mutations on L-type or T-type channels have been described yet to affect cortisol secretion or to be linked to the development of Cushing syndrome, but several evidences suggest that the function of T channels is also crucial in fasciculata cells. Putative molecular mechanisms and cellular structural organization making T channels a privileged entry for the “steroidogenic calcium” are also discussed.
Highlights
Voltage-operated calcium channels play a crucial role in signal transduction of many excitable and non-excitable cell types [1]
This early step in steroidogenesis is controlled by cytosolic and mitochondrial calcium levels as shown by several independent experimental observations: (a) rising ambient calcium stimulates aldosterone production in permeabilized glomerulosa cells and this response is prevented by the addition of ruthenium red, a blocker of the mitochondrial calcium uniporter [148], (b) intracellular calcium stimulates both intramitochondrial cholesterol transfer [150] and the expression of the steroidogenic acute regulatory (StAR) protein [151], which is required for efficient cholesterol transport into the mitochondria, and (c) cytosolic calcium fluctuations evoked by angiotensin II (AngII) are relayed and amplified within the mitochondrial matrix [152]
Rate limiting steps of steroidogenesis occurring within the mitochondria, and because calcium entering the cell through T channels is not detected within the cytosol of bovine adrenal glomerulosa cells [14], we have proposed that calcium is directly conveyed from the plasma membrane to the mitochondria via the lumen of the endoplasmic reticulum, which would act as a sort of “intracellular calcium pipeline” [112, 149] (Figure 3)
Summary
Channel: A Privileged Gate for Calcium Entry and Control of Adrenal Steroidogenesis. Calcium signaling has been shown to be more complex than initially thought It is confined within cell microdomains, and different calcium channels are associated with different functions, as shown by various channelopathies. Sporadic mutations on voltage-operated L-type calcium channels in adrenal glomerulosa cells have been shown recently to be the second most prevalent genetic abnormalities present in human aldosterone-producing adenoma. No similar mutations on L-type or T-type channels have been described yet to affect cortisol secretion or to be linked to the development of Cushing syndrome, but several evidences suggest that the function of T channels is crucial in fasciculata cells.
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