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Titlebook: Arterial Chemoreceptors; Arterial Chemorecept Constancio Gonzalez,Colin A. Nurse,Chris Peers Book 2009 The Editor(s) (if applicable) and Th

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Abdulla Al Neaimi,Philip Lutaayasence of KCN the CO donor increased wild-type channel activity in a concentration-dependent manner, with an EC. of ca. 50μM. Single cysteine point mutations of residues C820, C995 and C1028 affected neither channel characteristics nor CO EC. values. In contrast, the CO sensitivity of the C911G mutat
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Farouk Musa Aliyu,Adegboyega Ojoak K. conductance in rat type I cells remains unclear, but shares similarities with TASK-1 and TASK-3. Recombinant TASK-1 was insensitive to AICAR. However, TASK-3 was inhibited by either AICAR or A-769662 in a manner which was reversed by compound C. These data highlight a role for AMPK in the modu
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https://doi.org/10.1007/978-3-319-98827-6tion of DPPX to K. currents in rabbit CB chemoreceptor cells by using DPPX functional knockdown with siRNA. Our data suggest that DPPX proteins are integral components of K. currents, and that their association with Kv4 subunits modulate the pharmacological profile of the heteromultimers.
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Peterson Mwesiga,Julius Butime,Richard Okouoxic and 24 hours hypoxic cultured cells, acute hypoxic stimuli decreases NPo approximately 70% with no effects on current amplitude. On the other hand, in cultured cells subjected to 48 hours of hypoxia, NPo decreases near to 90% in response to acute hypoxia. We concluded that continuous hypoxic ex
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Nuove tecnologie a sostegno della didattica,ypoxic conditions in the absence of PDE inhibitors. In both conditions, the E. calculated for IBMX was similar to that of the specific PDE4 inhibitors. Hypoxia shifted the concentration response curves to the left with the following rank order of potency IBMX> RO 20-1724=rolipram and increased E. by
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