Attenuated Stress Response to Acute Restraint and Forced Swimming Stress in Arginine Vasopressin 1b Receptor Subtype (Avpr1b) Receptor Knockout Mice and Wild-Type Mice Treated with a Novel Avpr1b Receptor Antagonist

Rationale: Atrial natriuretic peptide (ANP) is stored in the heart in large dense core granules of atrial myocytes as a biologically inactive precursor, pro-ANP. Hemodynamic stress and atrial stretch stimulate coordinate secretion and proteolytic cleavage of pro-ANP to its bioactive form, ANP, which promotes renal salt excretion and vasodilation, which, together contribute to decreasing blood pressure. While the ATF6 branch of the ER stress response has been studied in ventricular tissue mouse models of myocardial ischemia and pathological hypertrophy, roles for ATF6 and ER stress on the endocrine function of atrial myocytes have not been studied. Objective/Methods: To address this gap in our knowledge, we knocked down ATF6 in primary cultured neonatal rat atrial myocytes (NRAMs) using a chemical inhibitor of the proteolytic cleavage site enabling ATF6 activation and siRNA and measured ANP expression and secretion basally and in response to alpha- adrenergic agonist stimulation using phenylephrine. We also compared the ANP secretion from wild- type mice and ATF6 knockout mice in an ex vivo Langendorff model of the isolated perfused heart. Results: ATF6 knockdown in NRAMs significantly impaired basal and phenylephrine-stimulated ANP secretion. ATF6 knockout mice displayed lower levels of ANP in atrial tissue at baseline as well as after phenylephrine treatment. Similarly, in the ex vivo isolated perfused heart model, less ANP was detected in effluent of ATF6 knockout hearts compared to wild-type hearts. Conclusions: The ATF6 branch of the ER stress response is necessary for efficient co-secretional processing of pro-ANP to ANP and for agonist-stimulated ANP secretion from atrial myocytes. As ANP is secreted in a regulated manner in response to a stimulus and pro-ANP is synthesized and packaged through the classical secretory pathway, we posit that ATF6 is required for adequate expression, folding, trafficking, processing and secretion of biologically active ANP from the endocrine heart.

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Swimming stress and adaptation by dystrophic and normal mice

American Journal of Physiology-Legacy Content ◽

10.1152/ajplegacy.1962.203.1.91 ◽

1962 ◽

Vol 203 (1) ◽

pp. 91-94 ◽

Cited By ~ 7

Author(s):

Hubert C. Soltan

Keyword(s):

Inbred Strain ◽

Swimming Speed ◽

Forced Swimming ◽

Swimming Stress ◽

The Cross ◽

Dystrophic Mice ◽

Forced Swimming Stress

Dystrophic mice, 5–11 weeks old, from the inbred strain 129/ Re- dy and from the cross between 129/Re- dy and the stock C57BL/6-Miwh/Re swam more slowly than normal littermates. For both normal and dystrophic mice the reduction in swimming speed after forced swimming stress was most marked in the first days of the new experience. No difference was detected in the swimming speeds of DyDy as compared with Dydy mice. But mice of both genotypes swam more rapidly when the temperature of the water was lowered from 95 F to 68 F.

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