C. J. Henderson scite author profile

C. J. Henderson

4Publications

36Citation Statements Received

0Citation Statements Given

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University of Auckland

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Immediate early gene transcription and synaptic modulation

et al. 1999

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Long-term changes in gene expression appear to be critical to the formation of memory, but little is known about its stimulus- transcription coupling. Numerous studies in the last decade, by focusing on unraveling this signal transduction pathway, have investigated the potential role of the immediate-early genes in this process. The krox family of immediate-early gene proteins are of particular interest because they may be involved in stabilizing the synaptic modifications that underlie hippocampal long-term potentiation (LTP). A potential upstream mediator of krox induction is cyclic AMP-responsive element binding protein (CREB), a posttranslationally activated transcription factor that has been implicated in numerous memory paradigms. In this study we investigated whether the activation of CREB by phosphorylation may have a role in the development of rat perforant- path-stimulated LTP and associated dentate granule cell krox-24 mRNA expression. Contrary to what was expected, we failed to show any difference in the levels of phosphorylated CREB after LTP or following endogenous synaptic facilitation stimulated by novelty. Using these same model systems we also investigated the protein levels of brain- derived neurotrophic factor (BDNF), another immediate-early gene that is induced following a durable form of LTP. However, BDNF protein was not induced within the hippocampus after LTP and was transiently decreased following novel environmental stimulation.

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The offset of β‐adrenoceptor antagonism of the responses of the rat right ventricle to isoprenaline

Doggrell

Henderson

1998

Journal of Autonomic Pharmacology

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1. The aim of the study was to test the hypothesis that the offset of action of beta-adrenoceptor antagonists on the heart is related to their lipophilicity, with low and highly lipophilic drugs having a rapid and slow offset, respectively. The effects of beta-blockers with low (atenolol), moderate (celiprolol), high (propranolol) and very high (bopindolol) lipophilicity on the contractile responses of the rat right ventricle to isoprenaline were determined. 2. Atenolol at 10(-6) and 10(-5) M, celiprolol at 10(-7), 10(-6) and 10(-5) M, propranolol at 10(-8), 10(-7) and 10(-6) M and bopindolol at 2 x 10(-9) and 10(-8) M caused parallel rightward shifts of the isoprenaline response curves with no effect on maximum responses. The Schild plots for atenolol, celiprolol and propranolol had slopes that were not significantly different from 1, which is indicative of competitive reversible antagonism. The pKB values were 7.33, 7.78, and 8.79 for atenolol, celiprolol, and propranolol, respectively. The Schild plot for bopindolol had a slope that was significantly greater than 1. 3. Our hypothesis is supported as the effects of propranolol and bopindolol were more slowly offset than those of atenolol and celiprolol. Thus, the concentration-ratio of 141 in the presence of atenolol at 10(-5) M was reduced to 4 after the first wash, whereas the ratio of 100 in the presence of propranolol at 10(-7) M was only reduced to 45 after a similar wash. The ratio of 54 with celiprolol at 10(-6) M was reduced to 5, whereas the ratio of 70 with bopindolol at 10(-8) M was only reduced to 28 by the first wash. 4. The effects of bopindolol were very slowly or not reversible over two washes in the absence or presence of atenolol at 10(-6) M. It is suggested that bopindolol is a very slowly reversible beta-blocker, and that this contributes to its slow offset of action.

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The effects of lignocaine and tetrodotoxin on the action potentials and contractions of left ventricles from normo- and hypertensive rats

Doggrell

Nand

Henderson

1999

General Pharmacology: The Vascular System

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The effects of bromoacetylalprenololmenthane on the responses to isoprenaline of the left ventricle from normo‐, prehyper‐ and hypertensive rats

Doggrell¹,

Mistry²,

Henderson³

1997

Journal of Autonomic Pharmacology

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1. We have studied the effects of bromoacetylalprenololmenthane (BAAM), a very slowly reversible beta-adrenoceptor antagonist, on the responses of the left ventricle of 5 and 22 week old Wistar Kyoto (WKY) rats and spontaneously hypertensive rats (SHRs) to isoprenaline. At 5 weeks the SHRs were prehypertensive and at 22 weeks they had hypertension-induced hypertrophy of the left ventricle. 2. The mean potency of isoprenaline on the left ventricle from 5 week old WKY was similar to that obtained on left ventricle with BAAM at 10(-6) M for 30 min, there was a parallel rightward shift of the isoprenaline concentration-response curves. Treatment with a higher concentration of BAAM (10(-5)M) caused non-parallel rightward shifts of the concentration-response curves, with a depression of the isoprenaline maximum responses. These data were used to derive affinity (KA) values for isoprenaline. The mean isoprenaline KA value on the left ventricle from 5 week old WKY was 2.44 x 10(-6)M, and similar KA values were obtained on the left ventricles from 22 week old WKY and 5 and 22 week old SHRs. On all the left ventricles tested, isoprenaline produced a half maximal response by occupying less than 1%, and a near maximal response by occupying about 5% of the available beta(1)-adrenoceptors. 4. This study has shown that there are no differences in the cardiac responses to isoprenaline at beta(1)-adrenoceptors, isoprenaline KA values or the beta(1)-adrenoceptor reserve for isoprenaline on the SHR left ventricle in prehypertension or in the early stages of hypertension-induced hypertrophy.

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C. J. Henderson

Immediate early gene transcription and synaptic modulation

The offset of β‐adrenoceptor antagonism of the responses of the rat right ventricle to isoprenaline

The effects of lignocaine and tetrodotoxin on the action potentials and contractions of left ventricles from normo- and hypertensive rats

The effects of bromoacetylalprenololmenthane on the responses to isoprenaline of the left ventricle from normo‐, prehyper‐ and hypertensive rats

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