David R. Livengood scite author profile

A B S TR A C T Depolarization of the presynaptic terminal by current produced a postsynaptic potential (PSP) which increased with increasing presynaptic polarization and then reached a plateau. Iontophoretic injection of tetraethylammonium ions (TEA) into the presynaptic axon near the terminal produced a prolonged presynaptic spike. The resulting PSP is increased in size and its time course closely followed that of the presynaptic spike. The presynaptic fiber no longer exhibited rectification and strong depolarizations revealed that the PSP reached a maximum with about 110 mv depolarization. Further depolarization produced a decrease in PSP amplitude and finally transmission was blocked. However, a PSP then always appeared on withdrawal of the depolarizing current. Under the conditions of these experiments, the PSP could be considered a direct measure of transmitter release. Bathing the TEA-injected synapse with concentrations of tetrodotoxin (TTX) sufficient to block spike activity in both pre-and postsynaptic axons did not greatly modify postsynaptic electrogenesis. However, doubling TTX concentration reversibly blocked PSP. Thus the permeability changes to Na and K accompanying the spike do not appear necessary for transmitter release. Some other processes related to the level of presynaptic polarization must be involved to explain the data. The inhibition of transmitter release by strong depolarizations appears to be related to Ca action. A membrane Ca current may also be necessary for normal transmitter release.

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Transformation of human osteoblast cells to the tumorigenic phenotype by depleted uranium-uranyl chloride.

Miller¹,

Blakely²,

Livengood³

et al. 1998

Environ Health Perspect

122

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Depleted uranium (DU) is a dense heavy metal used primarily in military applications. Although the health effects of occupational uranium exposure are well known, limited data exist regarding the long-term health effects of internalized DU in humans. We established an in vitro cellular model to study DU exposure. Microdosimetric assessment, determined using a Monte Carlo computer simulation based on measured intracellular and extracellular uranium levels, showed that few (0.0014%) cell nuclei were hit by alpha particles. We report the ability of DU-uranyl chloride to transform immortalized human osteoblastic cells (HOS) to the tumorigenic phenotype. DU-uranyl chloride-transformants are characterized by anchorage-independent growth, tumor formation in nude mice, expression of high levels of the k-ras oncogene, reduced production of the Rb tumor-suppressor protein, and elevated levels of sister chromatid exchanges per cell. DU-uranyl chloride treatment resulted in a 9.6 (+/- 2.8)-fold increase in transformation frequency compared to untreated cells. In comparison, nickel sulfate resulted in a 7.1 (+/- 2.1)-fold increase in transformation frequency. This is the first report showing that a DU compound caused human cell transformation to the neoplastic phenotype. Although additional studies are needed to determine if protracted DU exposure produces tumors in vivo, the implication from these in vitro results is that the risk of cancer induction from internalized DU exposure may be comparable to other biologically reactive and carcinogenic heavy-metal compounds (e.g., nickel).ImagesFigure 1Figure 2Figure 3

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Inward rectification in mouse macrophages: evidence for a negative resistance region

Gallin¹,

Livengood²

1981

American Journal of Physiology-Cell Physiology

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The electrical properties of cultured mouse thioglycollate-induced peritoneal macrophages were investigated using intracellular recording techniques. Thirty-five percent of the cells studied had membrane potentials ranging from -65 to -95 mV and exhibited S-shaped, steady-state current-voltage (I-V) relationships containing a transitional region. Analysis of currents in the transitional region from the rate of rise and fall of the voltage responses to current pulses indicated the presence of a negative resistance region in this area. Tetrodotoxin (3 X 10(-5) M), cobalt chloride (3 mM), 4-aminopyridine (4 mM), and tetraethylammonium chloride (8 mM) did not eliminate the transitional region of the I-V curves, whereas addition of barium chloride (4 mM) and rubidium chloride (3 mM) did. Increasing the external concentration of potassium shifted the I-V relationship horizontally along the current axis but did not eliminate the transitional region. These data indicate that the inward rectification and the negative resistance region probably result from a voltage-dependent potassium conductance.

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The action of vincaleukoblastine on mitosis in vitro

Palmer

Livengood

Warren

et al. 1960

Experimental Cell Research

141

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