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J. Biol. Chem., Vol. 265, Issue 15, 8444-8450, May, 1990
MT Nosek, DT Dransfield and JR Aprille
Adenine nucleotide transport over the carboxyatractyloside-insensitive
ATP-Mg/Pi carrier was assayed in isolated rat liver mitochondria with the
aim of investigating a possible regulatory role for Ca2+ on carrier
activity. Net changes in the matrix adenine nucleotide content (ATP + ADP +
AMP) occur when ATP-Mg exchanges for Pi over this carrier. The rates of net
accumulation and net loss of adenine nucleotides were inhibited when free
Ca2+ was chelated with EGTA and stimulated when buffered [Ca2+]free was
increased from 1.0 to 4.0 microM. The unidirectional components of net
change were similarly dependent on Ca2+; ATP influx and efflux were
inhibited by EGTA in a concentration- dependent manner and stimulated by
buffered free Ca2+ in the range 0.6- 2.0 microM. For ATP influx, increasing
the medium [Ca2+]free from 1.0 to 2.0 microM lowered the apparent Km for
ATP from 4.44 to 2.44 mM with no effect on the apparent Vmax (3.55 and 3.76
nmol/min/mg with 1.0 and 2.0 microM [Ca2+]free, respectively). Stimulation
of influx and efflux by [Ca2+]free was unaffected by either ruthenium red
or the Ca2+ ionophore A23187. Calmodulin antagonists inhibited transport
activity. In isolated hepatocytes, glucagon or vasopressin promoted an
increased mitochondrial adenine nucleotide content. The effect of both
hormones was blocked by EGTA, and for vasopressin, the effect was blocked
also by neomycin. The results suggest that the increase in mitochondrial
adenine nucleotide content that follows hormonal stimulation of hepatocytes
is mediated by an increase in cytosolic [Ca2+]free that activates the
ATP-Mg/Pi carrier.
Calcium stimulates ATP-Mg/Pi carrier activity in rat liver mitochondria
Department of Biology, Tufts University, Medford, Massachusetts 02155.
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