Sylvia A. Lappin scite author profile

Sylvia A. Lappin

5Publications

66Citation Statements Received

122Citation Statements Given

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116

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Queen's University Belfast

Publications

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Biphasic effects of hyposmotic challenge on excitation-contraction coupling in rat ventricular myocytes

Brette¹,

Calaghan

Lappin³

et al. 2000

American Journal of Physiology-Heart and Circulatory Physiology

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The effects of short (1 min) and long (7-10 min) exposure to hyposmotic solution on excitation-contraction coupling in rat ventricular myocytes were studied. After short exposure, the action potential duration at 90% repolarization (APD(90)), the intracellular Ca(2+) concentration ([Ca(2+)](i)) transient amplitude, and contraction increased, whereas the L-type Ca(2+) current (I(Ca, L)) amplitude decreased. Fractional sarcoplasmic reticulum (SR) Ca(2+) release increased but SR Ca(2+) load did not. After a long exposure, I(Ca,L), APD(90), [Ca(2+)](i) transient amplitude, and contraction decreased. The abbreviation of APD(90) was partially reversed by 50 microM DIDS, which is consistent with the participation of Cl(-) current activated by swelling. After 10-min exposure to hyposmotic solution in cells labeled with di-8-aminonaphthylethenylpyridinium, t-tubule patterning remained intact, suggesting the loss of de-t-tubulation was not responsible for the fall in I(Ca,L). After long exposure, Ca(2+) load of the SR was not increased, and swelling had no effect on the site-specific phosphorylation of phospholamban, but fractional SR Ca(2+) release was depressed. The initial positive inotropic response to hyposmotic challenge may be accounted for by enhanced coupling between Ca(2+) entry and release. The negative inotropic effect of prolonged exposure can be accounted for by shortening of the action potential duration and a fall in the I(Ca,L) amplitude.

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Oxygen-pulse curves in rat liver mitochondrial suspensions. Some observations and deductions

Archbold¹,

Farrington²,

Lappin³

et al. 1979

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1. The inference, implicit in the chemiosmotic hypothesis, that protons move into the bulk phase during ATP synthesis was investigated. 2. Incubation of rat liver mitochondria in the presence of the cation exchanger CM-Sephadex C-50 caused alkalinization in the medium, though total ATP synthesis remained unchanged. The addition of N-ethylmaleimide prevented the alkalinization, but there was still no indication of protons passing into the medium. The expected proton movement [Mitchell & Moyle (1967) Biochem. J. 105, 1147--1162] was readily detected when as an equivalent acid pulse. 3. Analysis of delta H+ decay curves after O2 pulses (3 micrograms-atoms of O/g of protein) indicated the presence of fast and slow components of decay, with first-order rate constants (k) of 0.24s-1 and 0.032s-1. The fast decay was finite and was eliminated in the presence of N-ethylmaleimide. 4. These observations are interpreted as evidence for the development of unmasking of fixed charges on the outer surface of the mitochondrial inner membrane during energization and for the existence of proton-retentive electrical fields (rho-zones) on this surface. The charge concentration is calculated as about 1 charge/10nm2. 5. A cycle of changes in a single fixed-charge molecule is proposed which mediates both Ca2+ uptake and the first step in the utilization of the rho-zone protonmotive force, delta p rho.

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A Study of Phosphorylation of the Measles Membrane Protein

Rima

Lappin

Roberts

et al. 1981

Journal of General Virology

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An extramitochondrial dimension

Lappin¹,

McKay

Malpress

1977

Trends in Biochemical Sciences

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Proton turnover at mitochondrial coupling sites

Lappin

Malpress

1980

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Sylvia A. Lappin

Biphasic effects of hyposmotic challenge on excitation-contraction coupling in rat ventricular myocytes

Oxygen-pulse curves in rat liver mitochondrial suspensions. Some observations and deductions

A Study of Phosphorylation of the Measles Membrane Protein

An extramitochondrial dimension

Proton turnover at mitochondrial coupling sites

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