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1. COmplexome Profiling ALignment (COPAL) reveals remodeling of mitochondrial protein complexes in Barth syndrome.

2. Barth syndrome cells display widespread remodeling of mitochondrial complexes without affecting metabolic flux distribution.

3. A homozygous missense mutation in ERAL1, encoding a mitochondrial rRNA chaperone, causes Perrault syndrome.

4. A sensitive mass spectrometry platform identifies metabolic changes of life history traits in C. elegans.

5. Tetracycline antibiotics impair mitochondrial function and its experimental use confounds research.

6. Prolonged daily light exposure increases body fat mass through attenuation of brown adipose tissue activity.

7. Cardiomyocyte-specific miRNA-30c over-expression causes dilated cardiomyopathy.

8. The two-faced progeria gene and its implications in aging and metabolism.

9. Deletion of the cardiolipin-specific phospholipase Cld1 rescues growth and life span defects in the tafazzin mutant: implications for Barth syndrome.

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