MITOCHONDRIAL
DYSFUNCTION IN BIPOLAR DISORDER
Tadafumi
Kato
Laboratory for Molecular Dynamics of Mental Disorders, Brain Science Institute,
RIKEN, Saitama, Japan
We
previously reported that energy metabolism was altered in the frontal lobes in
patients with bipolar disorder using phosphorus magnetic resonance spectroscopy
(31P-MRS). Recently, we found that decreased intracellular pH was
confirmed in the non-localized 31P-MR spectra of eh head, suggesting
that altered intracellular pH reflected the alteration of cellular metabolism in
bipolar disorder. Among the 31P-MRS findings of bipolar disorder,
significantly enhanced response of phosphocreatine (PCr) after the photic
stimulation in the occipital cortex was also reported in patients with
mitochondrial myopathy (chronic progressive external ophthalmoplegia, CPEO)
without central nervous system involvement. CPEO is caused by deletion of
mitochondrial DNA (mtDNA). There are three types of autosomal dominantly
inherited CPEO caused by mutations of POLG, ANT1, and Twinkle, all of which are
accompanied by depression or bipolar disorder. In addition, patients with
Wolfram disease, frequently accompanies bipolar disorder also have multiple
deletions of mtDNA in the brain. These findings altogether suggested that
bipolar disorder is related to mitochondrial dysfunction caused by accumulation
of mtDNA deletions.
We are
not studying the role of mitochondrial dysfunction in bipolar disorders using
several approaches. 1) Analysis of calcium signaling, mitochondrial membrane
potential, and complex I activity of transmitochondrial cybrids established from
platelets of bipolar disorder patients. 2) Association and gene expression
analysis of nuclear encoded mitochondrial complex I subunit genes. 3) Generation
of transgenic mice accumulating multiple deletion s of mtDNA. 4) Analysis of
whole mtDNA sequence in patients with bipolar disorder. 5) Quantification of
multiple deletions in the postmortem brains and lymphocytes. The preliminary
results of these studies confirmed our hypothesis that bipolar disorder is
associated with mitochondrial dysfunction.