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Fig. 3. Ste5p conformational models. Two models for how the binding of Gß{gamma} to Ste5p induces a conformational change in either (A) a folded dimer or (B) an anti-parallel dimer that is formed through interactions between the N- and C-terminal halves of Ste5p. The binding of the Gß{gamma} dimer (Ste4p and Ste18p) is postulated to align the associated kinases so as to permit serial phosphoryation. The models are adapted from (Sette et al., 2000); see text for details. Note that serial phosphorylations would occur in cis in model A and in trans in model B.





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