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Summary Cell pairs isolated from adult rat and guinea pig ventricles were used to study the electrical properties of the nexal membrane. Each cell of a pair was connected to a voltage-clamp system so as to enable whole-cell, tight-seal recording. The current-voltage relationship of the nexal membrane was found to be linear, revealing a resistance rn of 2–4 M. rn was insensitive to the sarcolemmal membrane potential (range:–90 to +30 mV), and exerted no time-dependent gating behavior (range: 0.1 to 10 s). Lowering pHi yielded a small increase in rn. Vigorous elevations in [Ca2+]i gave rise to an increase in rn which was associated with a cell shortening. Uncoupling caused by aliphatic alcohols or halothane did not produce cell shortening. Cell pairs were also used to study action potential transfer. 相似文献
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Different substrates were used to coat plastic petri dishes for the cultivation of dissociated fetal rat brain cells. Only on surfaces which were coated with a mixture of serum and non-reconstituted collagen, did the majority of the inoculated cells attach singly or as aggregates within 24 h. The attachment of the cells was followed by the outgrowth of cellular processes either from single cells or from aggregates in the same time period. This did not occur on collagen or serum treated or on regular plastic dishes. Under the latter conditions a similar outgrowth was observed only after 3–5 days. 相似文献
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A. S. Etienne E. Teroni R. Maurer V. Portenier F. Saucy 《Cellular and molecular life sciences : CMLS》1985,41(1):122-125
Summary When hoarding food under IR light, the golden hamster returns to its nest by path integration after an active outward journey, and it is capable of compensating the angular component of a passive outward journey independently of auditory, olfactory, tactile and geomagnetic cues. If, however, peripheral visual cues are available, they predominate over information which is gained during the active or passive outward journey. Further experiments show the limitations of homing by path integration, which is open to cumulative errors and therefore needs to be complemented by other categories of information.Acknowledgments. This research was supported by the Fonds national suisse de la recherche scientique, grants No. 3.349.0.74 and 3.753.0.80. We are very grateful to Dr J. Bovet, Dr W. Heiligenberg, Dr J. G. Mather and to an unknown referee for their critical comments and to Mr R. Schumacher for all his ingenious technical help. 相似文献
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Maurer M Wedemeyer J Metz M Piliponsky AM Weller K Chatterjea D Clouthier DE Yanagisawa MM Tsai M Galli SJ 《Nature》2004,432(7016):512-516
Endothelin-1 (ET-1) is a 21-amino-acid peptide, derived from vascular endothelial cells, with potent vasoconstrictor activity. ET-1 has been implicated in diverse physiological or pathological processes, including the vascular changes associated with sepsis. However, the factors that regulate ET-1-associated toxicity during bacterial infections, or in other settings, are not fully understood. Both the pathology associated with certain allergic and autoimmune disorders, and optimal host defence against bacterial and parasitic infections are mediated by mast cells. In vitro, mast cells can produce ET-1 (ref. 11), undergo ET-1-dependent and endothelin-A receptor (ET(A))-dependent activation, and release proteases that degrade ET-1 (ref. 14). Although the potential relationships between mast cells and the ET-1 system thus may be complex, the importance of interactions between ET-1 and mast cells in vivo is obscure. Here we show that ET(A)-dependent mast-cell activation can diminish both ET-1 levels and ET-1-induced pathology in vivo, and also can contribute to optimal survival during acute bacterial peritonitis. These findings identify a new biological function for mast cells: promotion of homeostasis by limiting the toxicity associated with an endogenous mediator. 相似文献