UV-triggered affinity capture identifies interactions between the Plasmodium falciparum multidrug resistance protein 1 (PfMDR1) and antimalarial agents in live parasitized cells

Voss, Till S.

doi:10.1074/jbc.m113.453159

UV-triggered affinity capture identifies interactions between the Plasmodium falciparum multidrug resistance protein 1 (PfMDR1) and antimalarial agents in live parasitized cells

Date Issued

2013-01-01

Author(s)

Brunner, R.

Ng, C. L.

Aissaoui, H.

Akabas, M. H.

Boss, C.

Brun, R.

Callaghan, P. S.

Corminboeuf, O.

Fidock, D. A.

Frame, I. J.

Heidmann, B.

Le Bihan, A.

Jeno, P.

Mattheis, C.

Moes, S.

Muller, I. B.

Paguio, M.

Roepe, P. D.

Siegrist, R.

Voss, Till S.

Welford, R. W.

Wittlin, S.

Binkert, C.

DOI

10.1074/jbc.m113.453159

Abstract

A representative of a new class of potent antimalarials with an unknown mode of action was recently described. To identify the molecular target of this class of antimalarials, we employed a photo-reactive affinity capture method to find parasite proteins specifically interacting with the capture compound in living parasitized cells. The capture reagent retained the antimalarial properties of the parent molecule (ACT-213615) and accumulated within parasites. We identified several proteins interacting with the capture compound and established a functional interaction between ACT-213615 and PfMDR1. We surmise that PfMDR1 may play a role in the antimalarial activity of the piperazine-containing compound ACT-213615.