Calcium channel blockers in vivo inhibit serotonin N‐acetyltransferase (NAT) activity in chicken retina stimulated by darkness and not by agents elevating intracellular cyclic AMP level

Zawilska, Jolanta B.; Wawrocka, Marlena; Zurawska, Ewa; Nowak, Jerzy Z.

doi:10.1111/j.1600-079x.1992.tb00062.x

Cited by 10 publications

(6 citation statements)

References 34 publications

(21 reference statements)

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“…However, such stimulatory effect has, to the best of our knowledge, never been shown before. On the contrary, other research groups have found decreased NAT activity (N-acetyltransferase, the rate-limiting enzyme step in MT biosynthesis) [36][37][38] when testing the effects of calcium channel blockers in other species. Meyer et al [39] treated baboons with intraperitoneal injections of the calcium antagonists verapamil, nifedipine, nitrendipine and nisoldipine.…”

Section: Discussionmentioning

confidence: 92%

Does hypercalcaemia or calcium antagonism affect human melatonin secretion or renal excretion?

Wikner

Wetterberg

Röjdmark

1997

Eur J Clin Investigation

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Patients with primary hyperparathyroidism have higher serum melatonin concentrations during active disease than after surgical cure. Whether this is caused by hypercalcaemia per se, increased parathyroid hormone secretion or other mechanisms is unknown. We decided to elucidate whether exogenous hypercalcaemia influences melatonin secretion. For this purpose, eight healthy volunteers were infused with calcium and saline on separate days and in random order (experiment A). Hypercalcaemia inhibited nocturnal melatonin secretion by 20% but left urinary melatonin excretion unaffected. If exogenous hypercalcaemia inhibits melatonin secretion, it is reasonable to assume that calcium channel blockers such as verapamil might have the opposite effect. This was investigated in experiment B, in which eight healthy subjects were treated on separate occasions with oral verapamil and placebo. Verapamil did not affect nocturnal melatonin secretion but increased melatonin excretion by 145%. As 6-sulphatoxy-melatonin is the main melatonin metabolite excreted by the kidneys, it was considered important to find out whether verapamil would also influence the excretion of 6-sulphatoxy-melatonin. This was investigated in experiment C, in which eight healthy volunteers were treated, on separate occasions, with oral verapamil and placebo. In this experiment also, verapamil increased urinary melatonin excretion significantly (by 67%), but left excretion of 6-sulphatoxy-melatonin unaffected. These findings imply that verapamil influences the renal and/or hepatic handling of melatonin.

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Section: Discussionmentioning

confidence: 92%

Does hypercalcaemia or calcium antagonism affect human melatonin secretion or renal excretion?

Wikner

Wetterberg

Röjdmark

1997

Eur J Clin Investigation

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“…L‐type calcium channel antagonists have been shown to suppress N ‐acetyltransferase activity at night in chicken retina, 10,29 regulating the synthesis of melatonin. The photoreceptors were well labelled with the antibody to α1d subunits, while they did not show immunoreactivity for α1c subunits and α1f subunits were localized to photoreceptor terminals.…”

Section: Discussionmentioning

confidence: 99%

“…In support of this, slowly inactivating L‐type calcium currents have been measured in many retinal cells, including photoreceptors, 1 horizontal cells, 2,3 bipolar cells 4–7 and Müller cells 8 . In addition, dihydropyridine antagonists, which block L‐type calcium channel function, block the release of glutamate in Xenopus photoreceptors, 9 and in chickens, the release of melatonin from photoreceptors is also regulated by an L‐type calcium current 10 …”

Section: Introductionmentioning

confidence: 86%

Localization of voltage‐sensitive L‐type calcium channels in the chicken retina

Firth

Morgan

Boelen

et al. 2001

Clinical Exper Ophthalmology

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L-type calcium channels have been associated with synaptic transmission in the retina, and are a potential site for modulation of the release of neurotransmitters. The present study documents the immunohistochemical localization of neuronal alpha1 subunits of L-type calcium channels in chicken retina, using antibodies to the alpha1c, alpha1d and alpha1f subunits of L-type calcium channels. The alpha1c-like subunits were localized to Müller cells, with predominantly radial processes, and a prominent band of horizontal processes in the outer plexiform layer. The antibody to alpha1d subunits labelled most, if not all, cell bodies. The antibody to a human alpha1f subunit strongly labelled photoreceptor terminals. Fainter immunoreactivity was detected in the inner segments of the photoreceptors, a subset of amacrine cells, two bands of labelling in the inner plexiform layer and many ganglion cells. The differential cellular distributons of these alpha1-subunits suggests subtle functional differences in their roles at different cellular locations.

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“…Although a role of calcium in the regulation of NAT activity and melatonin production as a result of alterations in intracellular concentrations of cyclic AMP has been suggested [Wilkinson, 1976;Zatz, 1989;Zawilska et al, 1992;Gasser and Gern, 1997], several lines of evidence indicate that calcium may regulate NAT activity and melatonin levels beyond the accumulation of cyclic AMP, i.e., affecting melatonin synthesis by directly regulating the production of NAT [Romero et al, 1975;Zatz and Romero, 1978;Harrison and Zatz, 1989;Zatz and Mullen, 1988;Zhan-Poe and Craft, 1999]. Under ordinary conditions, cyclic AMP mediates the induction of NAT by affecting both mRNA and protein synthesis [Romero et al, 1975;Zatz et al, 1976].…”

Section: Discussionmentioning

confidence: 99%

Role of extracellular calcium on the regulation of melatonin synthesis in the Syrian hamster pineal gland

Santana¹,

Sanchez²,

Reíter³

et al. 2001

Journal of Pineal Research

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The role of extracellular calcium on the induction of cyclic AMP production, N-acetyltransferase (NAT) activity and melatonin synthesis, induced by forskolin, was investigated in Syrian hamster pineal glands. Pineals were removed from hamsters killed either in the first half of the normal dark period or late in the dark period. Forskolin immediately increased NAT activity and melatonin levels only when the glands were collected late in the dark period, while in the first half of the dark phase, hamster pineals responded to forskolin with an increase of NAT activity and melatonin production only after 6 hr of incubation. The absence of calcium prevented the induction of melatonin synthesis by forskolin only when glands were collected early in the dark phase and incubated for 6 hr. In the second half of the normal dark period removal of calcium markedly decreased NAT activity and melatonin levels in glands incubated with forskolin for either 4 or 6 hr. However, the absence of extracellular calcium had no significant effect on the induction of cyclic AMP production by forskolin in pineals collected either early in the dark period or late in the dark phase. These data indicate that at least part of the action of extracellular calcium is indirect and that it affects steps in the induction of melatonin synthesis beyond the accumulation of cAMP.

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Calcium channel blockers in vivo inhibit serotonin N‐acetyltransferase (NAT) activity in chicken retina stimulated by darkness and not by agents elevating intracellular cyclic AMP level

Cited by 10 publications

References 34 publications

Does hypercalcaemia or calcium antagonism affect human melatonin secretion or renal excretion?

Does hypercalcaemia or calcium antagonism affect human melatonin secretion or renal excretion?

Localization of voltage‐sensitive L‐type calcium channels in the chicken retina

Role of extracellular calcium on the regulation of melatonin synthesis in the Syrian hamster pineal gland

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