Literature DB >> 12547789

Location of ryanodine and dihydropyridine receptors in frog myocardium.

Pierre Tijskens1, Gerhard Meissner, Clara Franzini-Armstrong.   

Abstract

Frog myocardium depends almost entirely on calcium entry from extracellular spaces for its beat-to-beat activation. Atrial myocardium additionally shows internal calcium release under certain conditions, but internal release in the ventricle is absent or very low. We have examined the content and distribution of the sarcoplasmic reticulum (SR) calcium release channels (ryanodine receptors, RyRs) and the surface membrane calcium channels (dihydropyridine receptors, DHPRs) in myocardium from the two atria and the ventricle of the frog heart using binding of radioactive ryanodine, immunolabeling of RyR and DHPR, and thin section and freeze-fracture electron microscopy. In cells from both types of chambers, the SR forms peripheral couplings and in both chambers peripheral couplings colocalize with clusters of DHPRs. However, although a low level of high affinity binding of ryanodine is detectable and RyRs are present in peripheral couplings of the atrium, the ventricle shows essentially no ryanodine binding and RyRs are not detectable either by electron microscopy or immunolabeling. The results are consistent with the lack of internal calcium release in the ventricle, and raise questions regarding the significance of DHPR at peripheral couplings in the absence of RyR. Interestingly, the free SR membrane in both heart chambers shows a low but equal density of intramembrane particles representing the Ca(2+) ATPase.

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Year:  2003        PMID: 12547789      PMCID: PMC1302685          DOI: 10.1016/S0006-3495(03)74924-8

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  73 in total

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6.  Sequential docking, molecular differentiation, and positioning of T-Tubule/SR junctions in developing mouse skeletal muscle.

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8.  Morphology and molecular composition of sarcoplasmic reticulum surface junctions in the absence of DHPR and RyR in mouse skeletal muscle.

Authors:  Edward Felder; Feliciano Protasi; Ronit Hirsch; Clara Franzini-Armstrong; Paul D Allen
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  14 in total

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7.  Differences in the control of basal L-type Ca(2+) current by the cyclic AMP signaling cascade in frog, rat, and human cardiac myocytes.

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8.  Expression and localization of ryanodine receptors in the frog semicircular canal.

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9.  Evolution of skeletal type e-c coupling: a novel means of controlling calcium delivery.

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10.  Ultrastructure of cardiac muscle in reptiles and birds: optimizing and/or reducing the probability of transmission between calcium release units.

Authors:  Stefano Perni; V Ramesh Iyer; Clara Franzini-Armstrong
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