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Pharmacological targeting of native CatSper channels reveals a required role in maintenance of sperm hyperactivation
- Source :
- PLoS ONE, PLoS ONE, Vol 4, Iss 8, p e6844 (2009)
- Publication Year :
- 2008
-
Abstract
- The four sperm-specific CatSper ion channel proteins are required for hyperactivated motility and male fertility, and for Ca(2+) entry evoked by alkaline depolarization. In the absence of external Ca(2+), Na(+) carries current through CatSper channels in voltage-clamped sperm. Here we show that CatSper channel activity can be monitored optically with the [Na(+)](i)-reporting probe SBFI in populations of intact sperm. Removal of external Ca(2+) increases SBFI signals in wild-type but not CatSper2-null sperm. The rate of the indicated rise of [Na(+)](i) is greater for sperm alkalinized with NH(4)Cl than for sperm acidified with propionic acid, reflecting the alkaline-promoted signature property of CatSper currents. In contrast, the [Na(+)](i) rise is slowed by candidate CatSper blocker HC-056456 (IC(50) approximately 3 microM). HC-056456 similarly slows the rise of [Ca(2+)](i) that is evoked by alkaline depolarization and reported by fura-2. HC-056456 also selectively and reversibly decreased CatSper currents recorded from patch-clamped sperm. HC-056456 does not prevent activation of motility by HCO(3) (-) but does prevent the development of hyperactivated motility by capacitating incubations, thus producing a phenocopy of the CatSper-null sperm. When applied to hyperactivated sperm, HC-056456 causes a rapid, reversible loss of flagellar waveform asymmetry, similar to the loss that occurs when Ca(2+) entry through the CatSper channel is terminated by removal of external Ca(2+). Thus, open CatSper channels and entry of external Ca(2+) through them sustains hyperactivated motility. These results indicate that pharmacological targeting of the CatSper channel may impose a selective late-stage block to fertility, and that high-throughput screening with an optical reporter of CatSper channel activity may identify additional selective blockers with potential for male-directed contraception.
- Subjects :
- Male
Developmental Biology/Germ Cells
lcsh:Medicine
Motility
chemistry.chemical_element
Calcium
03 medical and health sciences
Mice
0302 clinical medicine
Animals
lcsh:Science
Ion transporter
Ion channel
030304 developmental biology
0303 health sciences
030219 obstetrics & reproductive medicine
Multidisciplinary
Ion Transport
Hyperactivation
Voltage-dependent calcium channel
lcsh:R
Sodium
Depolarization
Anatomy
Sperm
Spermatozoa
chemistry
Biophysics
Physiology/Cell Signaling
lcsh:Q
Biophysics/Experimental Biophysical Methods
Calcium Channels
Research Article
Pharmacology/Drug Development
Subjects
Details
- ISSN :
- 19326203
- Volume :
- 4
- Issue :
- 8
- Database :
- OpenAIRE
- Journal :
- PloS one
- Accession number :
- edsair.doi.dedup.....32f716e46afaf75bc44c47d8200fec79