Drug and peptide transport in humans

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[[Morphs]] were generated with [https://fatcat.godziklab.org/ FATCAT], with the [https://proteopedia.org/cgi-bin/morph Proteopedia PyMOL Morpher], and with [[ChimeraX]]. The dipeptide ligand was absent in the FATCAT and Proteopedia/PyMOL morphs, but was retained in the ChimeraX morph PDB file. A ChimeraX morph between the isolated transmembrane domains, with hydrogen atoms deleted, was used for the above scenes, [[Image:7pmx-y-morph-chimerax-xmemb-noh.pdb.gz]].
[[Morphs]] were generated with [https://fatcat.godziklab.org/ FATCAT], with the [https://proteopedia.org/cgi-bin/morph Proteopedia PyMOL Morpher], and with [[ChimeraX]]. The dipeptide ligand was absent in the FATCAT and Proteopedia/PyMOL morphs, but was retained in the ChimeraX morph PDB file. A ChimeraX morph between the isolated transmembrane domains, with hydrogen atoms deleted, was used for the above scenes, [[Image:7pmx-y-morph-chimerax-xmemb-noh.pdb.gz]].
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Some steps in making the morph in ChimeraX are easily done from the menus, e.g. Tools, Structure Analysis, MatchMaker for superposition. Other steps must be done from commands. The complete command file for making a morph between the full-length PDB files is ''TO BE UPLOADED AND LINKED HERE''. The transmembrane domain PDB files were simply dragged and dropped into ChimeraX, instead of loading from the [[wwPDB]].
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Some steps in making the morph in ChimeraX are easily done from the menus, e.g. Tools, Structure Analysis, MatchMaker for superposition. Other steps must be done from commands. The complete command file for making a morph between the full-length PDB files is [https://proteopedia.org/wiki/images/a/a8/7pmx-y-morph.cxc 7pmx-y-morph.cxc]. The transmembrane domain PDB files were simply dragged and dropped into ChimeraX, instead of loading from the [[wwPDB]].

Revision as of 16:46, 11 December 2024

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References and Notes

  1. 1.0 1.1 1.2 1.3 1.4 1.5 Killer M, Wald J, Pieprzyk J, Marlovits TC, Low C. Structural snapshots of human PepT1 and PepT2 reveal mechanistic insights into substrate and drug transport across epithelial membranes. Sci Adv. 2021 Nov 5;7(45):eabk3259. doi: 10.1126/sciadv.abk3259. Epub 2021 Nov 3. PMID:34730990 doi:http://dx.doi.org/10.1126/sciadv.abk3259
  2. Shen J, Hu M, Fan X, Ren Z, Portioli C, Yan X, Rong M, Zhou M. Extracellular domain of PepT1 interacts with TM1 to facilitate substrate transport. Structure. 2022 Jul 7;30(7):1035-1041.e3. PMID:35580608 doi:10.1016/j.str.2022.04.011
  3. 2.0 Å pseudoatoms are called "extra fine detail" in PACUPP. It defaults to "fine" (3.0 Å), and also offers "very fine" (2.4 Å) or user-specified diameters.

Proteopedia Page Contributors and Editors (what is this?)

Eric Martz

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