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. 2015 Mar 23;10(3):e0119636. doi: 10.1371/journal.pone.0119636

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© 2015 Nguyen et al

This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.

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Fig 5 — Residue coloring scheme is similar to Fig. 3 (i.e. cyan sticks representation denotes MAPK specific residues and light orange/tan sticks denotes subfamily (e.g. JNK) specific residues). A) Interactions of the MAPK specific salt bridge in the apo, unphosphorylated p38α (PDBID: 1P38). B) Interactions of the corresponding region in phosphorylated, apo form of p38α (PDBID: 3PY3). C) Interactions of the salt bridge in ATP analog bound, dually phosphorylated state in p38γ (PDBID: 1CM8). D) Interactions in apo, unphosphorylated ERK5 (PDBID: 4IC8). E) Interactions in ATP analogue bound, unphosphorylated ERK5 (PDBID: 4IC7). F) Interactions in phosphorylated, ATP bound ERK2 (PDBID: 2ERK). G) Disengagement of canonical salt bridge in apo ERK2 (PDBID: 4GSB), where the side chains of E332^ERK2 and D334^ERK2 are disordered.