Belinda P. Johnson scite author profile

We investigated the shock initiation of energetic materials with a tabletop apparatus that uses km s−1 laser-driven flyer plates to initiate tiny explosive charges and obtains complete temperature histories with a high dynamic range. By comparing various microstructured formulations, including a pentaerythritol tetranitrate (PETN) based plastic explosive (PBX) denoted XTX-8003, we determined that micron-scale pores were needed to create high hot spot temperatures. In charges where micropores (i.e., micron-sized pores) were present, a hot spot temperature of 6000 K was observed; when the micropores were pre-compressed to nm scale, however, the hot spot temperature dropped to ∼4000 K. By comparing XTX-8003 with an analog that replaced PETN by nonvolatile silica, we showed that the high temperatures require gas in the pores, that the high temperatures were created by adiabatic gas compression, and that the temperatures observed can be controlled by the choice of ambient gases. The hot spots persist in shock-compressed PBXs even in vacuum because the initially empty pores became filled with gas created in-situ by shock-induced chemical decomposition.

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Observing Hot Spot Formation in Individual Explosive Crystals Under Shock Compression

Johnson

Zhou

Ihara

et al. 2020

J. Phys. Chem. A

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The formation of hot spots in dynamically compressed, plastic-bonded explosives is known to be the primary mechanism by which these materials ignite and initiate, but hot spots are small, fleeting, and hard to observe. Using a microscope equipped with laser-launched, miniflyer plates, we have studied hot spots in small grains of cyclotetramethylene-tetranitramine (HMX) embedded in a polyurethane binder, shocked to about 20 GPa. A nanosecond video with 4 μm spatial resolution is used to observe hot spot formation and growth, while nanosecond optical pyrometry measured temperature. Using individual ∼200 μm nominally single crystals of HMX (HMX-SC), we observed hot spots forming preferentially on corners or edges. These hot spots are about 4000 K. When there are multiple hot spots, the flame propagated along crystal edges, and the crystal is mostly combusted after about 300 ns. Using polycrystalline grains (HMX-PC), 6000 K hot spots are created near internal defects or crystal junctions. However, the thermal mass of the material at 6000 K is quite small, so after those hot spots cool down, the HMX combustion is similar to the single crystals. Comparing a HMX-based polymer-bonded explosive (PBX) to the individual polymer-bonded HMX-SC and HMX-PC grains shows that the myriad hot spots in the PBX are hotter than HMX-SC and colder than HMX-PC, but they persist for a longer time in PBX than in the individual grains.

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Inhibition of apoptosis by 60% oxygen: a novel pathway contributing to lung injury in neonatal rats

Man

Masood

Ziino

et al. 2011

American Journal of Physiology-Lung Cellular and Molecular Phys

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During early postnatal alveolar formation, the lung tissue of rat pups undergoes a physiological remodeling involving apoptosis of distal lung cells. Exposure of neonatal rats to severe hyperoxia (≥95% O(2)) both arrests lung growth and results in increased lung cell apoptosis. In contrast, exposure to moderate hyperoxia (60% O(2)) for 14 days does not completely arrest lung cell proliferation and is associated with parenchymal thickening. On the basis of similarities in lung architecture observed following either exposure to 60% O(2), or pharmacological inhibition of physiological apoptosis, we hypothesized that exposure to 60% O(2) would result in an inhibition of physiological lung cell apoptosis. Consistent with this hypothesis, we observed that the parenchymal thickening induced by exposure to 60% O(2) was associated with decreased numbers of apoptotic cells, increased expressions of the antiapoptotic regulator Bcl-xL, and the putative antiapoptotic protein survivin, and decreased expressions of the proapoptotic cleaved caspases-3 and -7. In summary, exposure of the neonatal rat lung to moderate hyperoxia results in an inhibition of physiological apoptosis, which contributes to the parenchymal thickening observed in the resultant lung injury.

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