Abstract
Correct regulation of cell contractility is critical for the function of many biological systems. The reproductive system of the hermaphroditic nematode C. elegans contains a contractile tube of myoepithelial cells known as the spermatheca, which stores sperm and is the site of oocyte fertilization. Regulated contraction of the spermatheca pushes the embryo into the uterus. Cell contractility in the spermatheca is dependent on actin and myosin and is regulated, in part, by Ca2+ signaling through the phospholipase PLC-1, which mediates Ca2+ release from the endoplasmic reticulum. Here, we describe a novel role for GSA-1/Gαs, and protein kinase A, composed of the catalytic subunit KIN-1/PKA-C and the regulatory subunit KIN-2/PKA-R, in the regulation of Ca2+ release and contractility in the C. elegans spermatheca. Without GSA-1/Gαs or KIN-1/PKA-C, Ca2+ is not released, and oocytes become trapped in the spermatheca. Conversely, when PKA is activated through either a gain of function allele in GSA-1 (GSA-1(GF)) or by depletion of KIN-2/PKA-R, the transit times and total numbers, although not frequencies, of Ca2+ pulses are increased, and Ca2+ propagates across the spermatheca even in the absence of oocyte entry. In the spermathecal-uterine valve, loss of GSA-1/Gαs or KIN-1/PKA-C results in sustained, high levels of Ca2+ and a loss of coordination between the spermathecal bag and sp-ut valve. Additionally, we show that depleting phosphodiesterase PDE-6 levels alters contractility and Ca2+ dynamics in the spermatheca, and that the GPB-1 and GPB-2 Gβ subunits play a central role in regulating spermathecal contractility and Ca2+ signaling. This work identifies a signaling network in which Ca2+ and cAMP pathways work together to coordinate spermathecal contractions for successful ovulations.
Highlights
Regulation of cellular contractility and relaxation is essential for the function of epithelial and endothelial tubes, which are subjected to changing flow, strain, and pressure as they transport liquid, gases, and other cells throughout the body [1,2]
GSA-1/Gαs and KIN-1/PKA is composed of two catalytic (PKA-C) are necessary for proper oocyte transit through the spermatheca
To determine if GSA-1/Gαs is required for oocyte transit, we depleted it using RNA interference (RNAi) in animals expressing GCaMP3 (GFP-calmodulin-M13 Peptide, version 3), a genetically encoded Ca2+ sensor, in the spermatheca [5,50]
Summary
Regulation of cellular contractility and relaxation is essential for the function of epithelial and endothelial tubes, which are subjected to changing flow, strain, and pressure as they transport liquid, gases, and other cells throughout the body [1,2]. The hermaphrodite reproductive system is composed of two symmetrical gonad arms surrounded by smooth muscle-like sheath cells, the spermathecae, and a common uterus [9,10]. Gonadal sheath cells contract and the distal neck of the spermatheca is pulled open to allow entry of the oocyte. After a regulated period of time the sp-ut valve opens and the distal spermathecal bag constricts to expel the embryo, [11,12]. Failure to coordinate these distinct contraction events during ovulation leads to embryos that fail to reach the uterus, become misshapen, or have decreased viability [4,7]
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