Identification of a Peptide Toxin from Grammostola spatulata Spider Venom That Blocks Cation-Selective Stretch-Activated Channels

Author:

Suchyna Thomas M.1,Johnson Janice H.2,Hamer Katherine2,Leykam Joseph F.3,Gage Douglas A.3,Clemo Henry F.4,Baumgarten Clive M.4,Sachs Frederick1

Affiliation:

1. From the Department of Physiology and Biophysics, State University of New York at Buffalo, Buffalo, New York 14214

2. NPS Pharmaceuticals, Inc., Salt Lake City, Utah 84108

3. Department of Biochemistry, Michigan State University–National Institutes of Health Mass Spectrometry Facility, Michigan State University, East Lansing, Michigan 48824-1319

4. Department of Internal Medicine and Physiology, Medical College of Virginia, Virginia Commonwealth University, Richmond, Virginia 23298

Abstract

We have identified a 35 amino acid peptide toxin of the inhibitor cysteine knot family that blocks cationic stretch-activated ion channels. The toxin, denoted GsMTx-4, was isolated from the venom of the spider Grammostola spatulata and has <50% homology to other neuroactive peptides. It was isolated by fractionating whole venom using reverse phase HPLC, and then assaying fractions on stretch-activated channels (SACs) in outside-out patches from adult rat astrocytes. Although the channel gating kinetics were different between cell-attached and outside-out patches, the properties associated with the channel pore, such as selectivity for alkali cations, conductance (∼45 pS at −100 mV) and a mild rectification were unaffected by outside-out formation. GsMTx-4 produced a complete block of SACs in outside-out patches and appeared specific since it had no effect on whole-cell voltage-sensitive currents. The equilibrium dissociation constant of ∼630 nM was calculated from the ratio of association and dissociation rate constants. In hypotonically swollen astrocytes, GsMTx-4 produces ∼40% reduction in swelling-activated whole-cell current. Similarly, in isolated ventricular cells from a rabbit dilated cardiomyopathy model, GsMTx-4 produced a near complete block of the volume-sensitive cation-selective current, but did not affect the anion current. In the myopathic heart cells, where the swell-induced current is tonically active, GsMTx-4 also reduced the cell size. This is the first report of a peptide toxin that specifically blocks stretch-activated currents. The toxin affect on swelling-activated whole-cell currents implicates SACs in volume regulation.

Publisher

Rockefeller University Press

Subject

Physiology

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