Interleukin 3‐stimulated proliferation is sensitive to pertussis toxin: Evidence for a guanyl nucleotide regulatory protein‐mediated signal transduction mechanism

David J. Kelvin; M. Shreeve; C. McAuley; D. L. McLeod; G. Simard; J. A. Connolly

doi:10.1002/jcp.1041380208

Interleukin 3‐stimulated proliferation is sensitive to pertussis toxin: Evidence for a guanyl nucleotide regulatory protein‐mediated signal transduction mechanism

David J. Kelvin, M. Shreeve, C. McAuley, D. L. McLeod, G. Simard, J. A. Connolly

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16 Citations (Scopus)

Résumé

Interleukin 3 (IL‐3) stimulates several biochemical and biological responses in IL‐3‐dependent tissue culture cells. We examined the possibility that guanyl nucleotide regulatory (G) proteins may transduce signals from IL‐3 receptors. We report here that pertussis toxin (PT), which can covalently modify a subclass of G proteins, is capable of inhibiting IL‐3‐stimulated proliferation in a dose‐dependent fashion. PT inhibiton of IL‐3‐stimulated proliferation could be overcome by using the Ca^{+ +} ionophore A23187 in conjunction with TPA. PT could also inhibit IL‐3‐stimulated hexose transport. In the absence of IL‐3, hexose transport could be stimulated by introducing GTPγS into intact cells. From these data we propose that IL‐3 receptors transduce signals via a PT‐sensitive G protein(s).

Langue d'origine	English
Pages (de-à)	273-280
Nombre de pages	8
Journal	Journal of Cellular Physiology
Volume	138
Numéro de publication	2
DOI	https://doi.org/10.1002/jcp.1041380208
Statut de publication	Published - févr. 1989
Publié à l'externe	Oui

ASJC Scopus Subject Areas

Physiology
Clinical Biochemistry
Cell Biology

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10.1002/jcp.1041380208

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abstract = "Interleukin 3 (IL‐3) stimulates several biochemical and biological responses in IL‐3‐dependent tissue culture cells. We examined the possibility that guanyl nucleotide regulatory (G) proteins may transduce signals from IL‐3 receptors. We report here that pertussis toxin (PT), which can covalently modify a subclass of G proteins, is capable of inhibiting IL‐3‐stimulated proliferation in a dose‐dependent fashion. PT inhibiton of IL‐3‐stimulated proliferation could be overcome by using the Ca+ + ionophore A23187 in conjunction with TPA. PT could also inhibit IL‐3‐stimulated hexose transport. In the absence of IL‐3, hexose transport could be stimulated by introducing GTPγS into intact cells. From these data we propose that IL‐3 receptors transduce signals via a PT‐sensitive G protein(s).",

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AU - McLeod, D. L.

AU - Simard, G.

AU - Connolly, J. A.

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Interleukin 3‐stimulated proliferation is sensitive to pertussis toxin: Evidence for a guanyl nucleotide regulatory protein‐mediated signal transduction mechanism

Résumé

ASJC Scopus Subject Areas

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