Dopamine transporter oligomerization: impact of combining protomers with differential cocaine analog binding affinities

Zhen, Juan; Antonio, Tamara; Cheng, Shu‐Yuan; Ali, Solav; Jones, Kymry T.; Reith, Maarten E. A.

doi:10.1111/jnc.13025

Cited by 32 publications

(38 citation statements)

References 33 publications

(77 reference statements)

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“…Dominant negative mutants of the human dopamine transporter (DAT) have been shown to reduce the function of co-expressed WT transporters, without any effect on trafficking to the plasma membrane [22]. Further functional studies have supported co-operativity, or cross-talk, between individual protomers in DAT oligomers [23]. Additional supportive evidence for this cross-talk has come from studies on fusion proteins of the serotonin transporter (SERT) with GAT-1 [24].…”

Section: The Leut Superfamilymentioning

confidence: 99%

Transporter oligomerization: form and function

Alguel

Cameron

Diallinas

et al. 2016

Biochemical Society Transactions

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Transporters are integral membrane proteins with central roles in the efficient movement of molecules across biological membranes. Many transporters exist as oligomers in the membrane. Depending on the individual transport protein, oligomerization can have roles in membrane trafficking, function, regulation and turnover. For example, our recent studies on UapA, a nucleobase ascorbate transporter, from Aspergillus nidulans, have revealed both that dimerization of this protein is essential for correct trafficking to the membrane and the structural basis of how one UapA protomer can affect the function of the closely associated adjacent protomer. Here, we review the roles of oligomerization in many particularly well-studied transporters and transporter families.

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Section: The Leut Superfamilymentioning

confidence: 99%

Transporter oligomerization: form and function

Alguel

Cameron

Diallinas

et al. 2016

Biochemical Society Transactions

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“…Our previous study demonstrated an influence of DAT protomer composition on the properties of a DAT inhibitor (Zhen et al . ). When DAT oligomers contained combinations of certain protomers with differential affinity for the cocaine phenyltropane analog CFT ((‐)‐2‐β‐carbomethoxy‐3‐β‐(4‐fluorophenyl) tropane = WIN 35 428), the resulting binding affinity differed from that found under conditions where heterooligomers were not present.…”

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confidence: 97%

Functional properties of dopamine transporter oligomers after copper linking

Zhen

Reith

2017

Journal of Neurochemistry

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Although it is universally accepted that dopamine transporters (DATs) exist in monomers, dimers and tetramers (i.e. dimers of dimers), it is not known whether the oligomeric organization of DAT is a prerequisite for its ability to take up dopamine (DA), or whether each DAT protomer, the subunit of quaternary structure, functions independently in terms of DA translocation. In this study, copper phenanthroline (CuP) was used to selectively target surface DAT: increasing concentrations of CuP gradually cross-linked natural DAT dimers in LLC-PK cells stably expressing hDAT and thereby reduced DA uptake functionality until all surface DATs were inactivated. DATs that were not cross-linked by CuP showed normal DA uptake with DA K at ~ 0.5 μM and DA efflux with basal and amphetamine-induced DA efflux as much as control values. The cocaine analog 2β-carbomethoxy-3β-[4-fluorophenyl]-tropane (CFT) was capable to bind to copper-cross-linked DATs, albeit with an affinity more than fivefold decreased (K of CFT = 109 nM after cross-linking vs 19 nM before). A kinetic analysis is offered describing the changing amounts of dimers and monomers with increasing [CuP], allowing the estimation of dimer functional activity compared with a DAT monomer. Consonant with previous conclusions for serotonin transporter and NET that only one protomer of an oligomer is active at the time, the present data indicated a functional activity of the DAT dimer of 0.74 relative to a monomer.

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“…Whether oligomeric complexes are the predominant state of DAT orientation in vivo is unknown, but some evidence supports the existence of DAT tetramers within striatal membranes (Milner et al, 1994). However, the potential significance of oligomers has been demonstrated by recent work showing that, under certain conditions, DAT protomers within an oligomeric complex affect the conformational state of one another, altering DA transport activity and sensitivity to stimulants historically classified as DAT reuptake inhibitors such as cocaine (Zhen et al, 2015). The size, composition, and distribution of DAT oligomeric complexes may therefore influence the sensitivity of particular dopaminergic neurons to stimulants and any subsequent toxicity.…”

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confidence: 99%