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Manju A. Kurian, Juan Zhen, Shu-Yuan Cheng, Yan Li, Santosh R. Mordekar, Philip Jardine, Neil V. Morgan, Esther Meyer, Louise Tee, Shanaz Pasha, Evangeline Wassmer, Simon J.R. Heales, Paul Gissen, Maarten E.A. Reith, Eamonn R. Maher
Published in Volume 119, Issue 6
J Clin Invest. 2009; 119(6):1595–1603 doi:10.1172/JCI39060
Abstract | Full text | PDF
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Figure 8
Two-dimensional representation of DAT topology based on LeuT structure.

Twelve transmembrane domains are shown with helically unwound regions in the first and sixth domain; extracellular and intracellular loops include helical portions (e2, e3, e4a, e4b, and i1, i5, respectively) (10, 11). Leu368 (L; red), subject to missense mutation, is shown at the top of transmembrane domain 7, one helix turn under Met371 (M; blue). Pro395 (P; red), also subject to missense mutation, is shown in the e4b portion of extracellular loop 4, one helix turn above Ala399 (A; blue). In the 3-dimensional structure, sodium ions interact not only with residues of transmembrane domains 1, 6, and 8, but also with transmembrane domain 7 (10).