The ADP/ATP carrier is the 32-kilodalton receptor for an NH2-terminally myristylated src peptide but not for pp60src polypeptide.

Abstract: Membrane binding of pp60src is initiated via its myristylated NH2 terminus. To identify a candidate pp6G' docking protein or receptor in the membrane, a radiolabelled peptide corresponding to the pp6tO' NH2-terminal membrane binding domain was cross-linked to fibroblast membranes and found to specifically label a 32-kDa protein. This protein was purified by appending an affinity tag to the peptide probe so that the cross-linked complex could be isolated via affinity chromatography. Microsequencing indicated th… Show more

“…Cell surface topology of ANT So far, only three studies on Leishmania, murine fibroblasts, and breast carcinoma and fibrosarcoma cells provide solid evidence that ANT is not only localized in mitochondria, but also at the cell surface (Sigal and Resh, 1993;Detke and Elsabrouty, 2008;Radichev et al, 2009). Our study confirms these findings and shows that the three ANT loops that project into the lumen of mitochondria are exposed at the neuronal cell surface (Fig.…”

“…Since it has been reported that ANT is located at the plasma membrane of Leishmania, fibroblasts, and cancer cells (Sigal and Resh, 1993;Detke and Elsabrouty, 2008;Radichev et al, 2009), and since we demonstrated that ANT interacts with the extracellular domain of L1, we tested whether ANT1 and/or ANT2 are present at the cell surface of cultured cerebellar neurons. Therefore, live primary cultures of cerebellar neurons were subjected to cell surface biotinylation, and biotinylated proteins were isolated using streptavidin-conjugated beads.…”

The Interaction between Cell Adhesion Molecule L1, Matrix Metalloproteinase 14, and Adenine Nucleotide Translocator at the Plasma Membrane Regulates L1-Mediated Neurite Outgrowth of Murine Cerebellar Neurons

“…Cell surface topology of ANT So far, only three studies on Leishmania, murine fibroblasts, and breast carcinoma and fibrosarcoma cells provide solid evidence that ANT is not only localized in mitochondria, but also at the cell surface (Sigal and Resh, 1993;Detke and Elsabrouty, 2008;Radichev et al, 2009). Our study confirms these findings and shows that the three ANT loops that project into the lumen of mitochondria are exposed at the neuronal cell surface (Fig.…”

“…Since it has been reported that ANT is located at the plasma membrane of Leishmania, fibroblasts, and cancer cells (Sigal and Resh, 1993;Detke and Elsabrouty, 2008;Radichev et al, 2009), and since we demonstrated that ANT interacts with the extracellular domain of L1, we tested whether ANT1 and/or ANT2 are present at the cell surface of cultured cerebellar neurons. Therefore, live primary cultures of cerebellar neurons were subjected to cell surface biotinylation, and biotinylated proteins were isolated using streptavidin-conjugated beads.…”

The Interaction between Cell Adhesion Molecule L1, Matrix Metalloproteinase 14, and Adenine Nucleotide Translocator at the Plasma Membrane Regulates L1-Mediated Neurite Outgrowth of Murine Cerebellar Neurons

“…63 However, at present it is not clear whether Figure 1 Molecules influencing ANT-mediated pore formation in chemically defined systems. The upper part lists proteins affecting the pore function of ANT, whereas the lower part focuses on non-protein molecules.…”

Permeabilization of the mitochondrial inner membrane during apoptosis: impact of the adenine nucleotide translocator

“…Crosslinking experiments identified a 32-kDa protein as the major species labeled by a myristoylated amino-terminal Src peptide probe (12,13). However, upon purification, this protein was found to be the ADP/ATP carrier, a mitochondrial protein capable of binding myristoyl-Src peptide but not the Src protein (14). To date no other protein has been identified as a binding partner for the Src amino terminus.…”

Amino-terminal basic residues of Src mediate membrane binding through electrostatic interaction with acidic phospholipids.