Fatty acid oxidation by the osteoblast is required for normal bone acquisition in a sex- and diet-dependent manner
Soohyun P. Kim, … , Michael J. Wolfgang, Ryan C. Riddle
Soohyun P. Kim, … , Michael J. Wolfgang, Ryan C. Riddle
Published August 17, 2017
Citation Information: JCI Insight. 2017;2(16):e92704. https://doi.org/10.1172/jci.insight.92704.
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Research Article Bone biology

Fatty acid oxidation by the osteoblast is required for normal bone acquisition in a sex- and diet-dependent manner

Abstract

Postnatal bone formation is influenced by nutritional status and compromised by disturbances in metabolism. The oxidation of dietary lipids represents a critical source of ATP for many cells but has been poorly studied in the skeleton, where the prevailing view is that glucose is the primary energy source. Here, we examined fatty acid uptake by bone and probed the requirement for fatty acid catabolism during bone formation by specifically disrupting the expression of carnitine palmitoyltransferase 2 (Cpt2), an obligate enzyme in fatty acid oxidation, in osteoblasts and osteocytes. Radiotracer studies demonstrated that the skeleton accumulates a significant fraction of postprandial fatty acids, which was equal to or in excess of that acquired by skeletal muscle or adipose tissue. Female, but not male, Cpt2 mutant mice exhibited significant impairments in postnatal bone acquisition, potentially due to an inability of osteoblasts to modify fuel selection. Intriguingly, suppression of fatty acid utilization by osteoblasts and osteocytes also resulted in the development of dyslipidemia and diet-dependent modifications in body composition. Taken together, these studies demonstrate a requirement for fatty acid oxidation during bone accrual and suggest a role for the skeleton in lipid homeostasis.

Authors

Soohyun P. Kim, Zhu Li, Meredith L. Zoch, Julie L. Frey, Caitlyn E. Bowman, Priyanka Kushwaha, Kathleen A. Ryan, Brian C. Goh, Susanna Scafidi, Julie E. Pickett, Marie-Claude Faugere, Erin E. Kershaw, Daniel L. J. Thorek, Thomas L. Clemens, Michael J. Wolfgang, Ryan C. Riddle

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Figure 2

Fatty acid oxidation is required for the maintenance of normal bone structure in female mice.

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Fatty acid oxidation is required for the maintenance of normal bone stru...
(A) qPCR analysis of Cpt2 mRNA levels in the femur of 6-week-old control and ΔCpt2 mice (n = 5–7 mice). (B) Body weight was assessed weekly from 3–12 weeks of age (n = 7–11 mice). (C and D) Quantification of trabecular bone volume in the distal femur (C) and L5 vertebrae (D) of male control and ΔCpt2 mice (n = 6–12 mice). (E) Representative computer renderings of bone structure in the distal femur (top), L5 vertebrae (middle), and femoral mid-diaphysis (bottom) of 6-week-old female control and ΔCpt2 mice. (F–I) Quantification of trabecular bone volume per tissue volume (F and H, BV/TV), trabecular number (G and I, Tb.N) in the distal femur (F and G) and L5 vertebrae (H and I) of female control and ΔCpt2 mice (n = 7–11 mice). (J–L) Quantification of cortical tissue area (J, Tt.Ar), cortical thickness (K, Ct.Th), and cortical area per tissue area (L, Ct.Ar/Tt.Ar) at the mid-diaphysis of female control and ΔCpt2 mice (n = 7–10 mice). All data are represented by mean ± SEM. *P < 0.05 by unpaired, two-tailed Student’s t test.