Literature DB >> 19759014

Demonstration and characterization of the heterodimerization of ZnT5 and ZnT6 in the early secretory pathway.

Ayako Fukunaka1, Tomoyuki Suzuki, Yayoi Kurokawa, Tomohiro Yamazaki, Naoko Fujiwara, Kaori Ishihara, Hitoshi Migaki, Katsuzumi Okumura, Seiji Masuda, Yuko Yamaguchi-Iwai, Masaya Nagao, Taiho Kambe.   

Abstract

The majority of CDF/ZnT zinc transporters form homo-oligomers. However, ZnT5, ZnT6, and their orthologues form hetero-oligomers in the early secretory pathway where they load zinc onto zinc-requiring enzymes and maintain secretory pathway functions. The details of this hetero-oligomerization remain to be elucidated, and much more is known about homo-oligomerization that occurs in other CDF/ZnT family proteins. Here, we addressed this issue using co-immunoprecipitation experiments, mutagenesis, and chimera studies of hZnT5 and hZnT6 in chicken DT40 cells deficient in ZnT5, ZnT6, and ZnT7 proteins. We found that hZnT5 and hZnT6 combine to form heterodimers but do not form complexes larger than heterodimers. Mutagenesis of hZnT6 indicated that the sites present in transmembrane domains II and V in which many CDF/ZnT proteins have conserved hydrophilic amino acid residues are not involved in zinc binding of hZnT6, although they are required for zinc transport in other CDF/ZnT family homo-oligomers. We also found that the long N-terminal half of hZnT5 is not necessary for its functional interaction with hZnT6, whereas the cytosolic C-terminal tail of hZnT5 is important in determining hZnT6 as a partner molecule for heterodimer formation. In DT40 cells, cZnT5 variant lacking the N-terminal half was endogenously induced during periods of endoplasmic reticulum stress and so seemed to function to supply zinc to zinc-requiring enzymes under these conditions. The results outlined here provide new information about the mechanism of action through heterodimerization of CDF/ZnT proteins that function in the early secretory pathway.

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Year:  2009        PMID: 19759014      PMCID: PMC2781478          DOI: 10.1074/jbc.M109.026435

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  39 in total

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4.  The yeast gene MSC2, a member of the cation diffusion facilitator family, affects the cellular distribution of zinc.

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5.  Functional characterization of a novel mammalian zinc transporter, ZnT6.

Authors:  Liping Huang; Catherine P Kirschke; Jane Gitschier
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6.  Biochemical properties of vacuolar zinc transport systems of Saccharomyces cerevisiae.

Authors:  Colin W MacDiarmid; Mark A Milanick; David J Eide
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7.  An antiport mechanism for a member of the cation diffusion facilitator family: divalent cations efflux in exchange for K+ and H+.

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Review 8.  Mammalian zinc transporters: nutritional and physiologic regulation.

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9.  ZnT7, a novel mammalian zinc transporter, accumulates zinc in the Golgi apparatus.

Authors:  Catherine P Kirschke; Liping Huang
Journal:  J Biol Chem       Date:  2002-11-21       Impact factor: 5.157

10.  A novel zinc-regulated human zinc transporter, hZTL1, is localized to the enterocyte apical membrane.

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  44 in total

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2.  Altered expression of two zinc transporters, SLC30A5 and SLC30A6, underlies a mammary gland disorder of reduced zinc secretion into milk.

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3.  In situ dimerization of multiple wild type and mutant zinc transporters in live cells using bimolecular fluorescence complementation.

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Review 4.  Evidence for operation of the direct zinc ligand exchange mechanism for trafficking, transport, and reactivity of zinc in mammalian cells.

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5.  Heterodimerization, altered subcellular localization, and function of multiple zinc transporters in viable cells using bimolecular fluorescence complementation.

Authors:  Yarden Golan; Bluma Berman; Yehuda G Assaraf
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Review 6.  Physiological roles of zinc transporters: molecular and genetic importance in zinc homeostasis.

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8.  A dominant negative heterozygous G87R mutation in the zinc transporter, ZnT-2 (SLC30A2), results in transient neonatal zinc deficiency.

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9.  Mutations in SLC30A10 cause parkinsonism and dystonia with hypermanganesemia, polycythemia, and chronic liver disease.

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10.  X-ray fluorescence microscopy reveals accumulation and secretion of discrete intracellular zinc pools in the lactating mouse mammary gland.

Authors:  Nicholas McCormick; Vanessa Velasquez; Lydia Finney; Stefan Vogt; Shannon L Kelleher
Journal:  PLoS One       Date:  2010-06-11       Impact factor: 3.240

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