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Volume 270,
Number 35,
Issue of September 01, pp. 20285-20291, 1995
©1995 by The American Society for Biochemistry and Molecular Biology, Inc.
Identification
and Purification of a 10-Kilodalton Protein Associated with
Mitochondrial Benzodiazepine Receptors
(Received for publication, November 16, 1994; and in revised form, May 15, 1995 )
Jaroslav Blahos
II,
Michael
E.
Whalin,
Karl E.
Krueger
The isoquinoline carboxamide photoaffinity probe PK14105, a
ligand with selectivity for mitochondrial benzodiazepine receptors, has
been established to photolabel an 18-kDa protein. When this radioactive
probe is used to photolabel rat mitochondrial preparations, a protein
of 10 kDa, in addition to the 18-kDa protein, is identified following
electrophoretic separation and extended autoradiography. These proteins
are referred to herein as pk10 and pk18, respectively. Both proteins
exhibited the same specificity to a series of ligands used in
competition photolabeling studies and are mutually present at
apparently similar ratios across multiple tissues. Subcellular
fractionation of rat adrenals indicated that pk10 and pk18 comigrated
with the mitochondrial marker enzyme cytochrome c oxidase. In
numerous paradigms examining specificity, photolabeling of pk18
invariably coincided with photolabeling of pk10. In
detergent-solubilized extracts of rat adrenal mitochondria, pk18 and
pk10 coimmunoprecipitated when using antisera raised against pk18.
Furthermore, purification of the photolabeled proteins using
nondenaturing conditions demonstrated that pk18 and pk10 copurify
substantiating their intimate association. A set of three antisera,
specific to different regions of pk18, did not recognize pk10 on
Western blots. Likewise, partial amino acid sequence of peptide
fragments indicate that pk10 is not derived from proteolytic cleavage
of pk18. These data suggest that pk10 represents another component of
mitochondrial benzodiazepine receptors whose identity is not apparent
with any known protein.

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Copyright © 1995 by the American Society for Biochemistry and Molecular Biology.
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