Vitamin B12-dependent taurine synthesis regulates growth and bone mass

Pablo Roman-Garcia; Isabel Quiros-Gonzalez; Lynda Mottram; Liesbet Lieben; Kunal Sharan; Arporn Wangwiwatsin; Jose Tubio; Kirsty Lewis; Debbie Wilkinson; Balaji Santhanam; Nazan Sarper; Simon Clare; George S. Vassiliou; Vidya R. Velagapudi; Gordon Dougan; Vijay K. Yadav

doi:10.1172/JCI72606

Vitamin B₁₂-dependent taurine synthesis regulates growth and bone mass

Pablo Roman-Garcia, Isabel Quiros-Gonzalez, Lynda Mottram, Liesbet Lieben, Kunal Sharan, Arporn Wangwiwatsin, Jose Tubio, Kirsty Lewis, Debbie Wilkinson, Balaji Santhanam, Nazan Sarper, Simon Clare, George S. Vassiliou, Vidya R. Velagapudi, Gordon Dougan, Vijay K. Yadav^*

^*Corresponding author for this work

Medical Sciences

Research output: Contribution to journal › Article › peer-review

108 Citations (Scopus)

Abstract

Both maternal and offspring-derived factors contribute to lifelong growth and bone mass accrual, although the specific role of maternal deficiencies in the growth and bone mass of offspring is poorly understood. In the present study, we have shown that vitamin B₁₂ (B₁₂) deficiency in a murine genetic model results in severe postweaning growth retardation and osteoporosis, and the severity and time of onset of this phenotype in the offspring depends on the maternal genotype. Using integrated physiological and metabolomic analysis, we determined that B₁₂ deficiency in the offspring decreases liver taurine production and associates with abrogation of a growth hormone/insulin-like growth factor 1 (GH/IGF1) axis. Taurine increased GH-dependent IGF1 synthesis in the liver, which subsequently enhanced osteoblast function, and in B₁₂-deficient offspring, oral administration of taurine rescued their growth retardation and osteoporosis phenotypes. These results identify B₁₂ as an essential vitamin that positively regulates postweaning growth and bone formation through taurine synthesis and suggests potential therapies to increase bone mass.

Original language	English
Pages (from-to)	2988-3002
Number of pages	15
Journal	Journal of Clinical Investigation
Volume	124
Issue number	7
DOIs	https://doi.org/10.1172/JCI72606
Publication status	Published - 1 Jul 2014

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Roman-Garcia, P., Quiros-Gonzalez, I., Mottram, L., Lieben, L., Sharan, K., Wangwiwatsin, A., Tubio, J., Lewis, K., Wilkinson, D., Santhanam, B., Sarper, N., Clare, S., Vassiliou, G. S., Velagapudi, V. R., Dougan, G., & Yadav, V. K. (2014). Vitamin B₁₂-dependent taurine synthesis regulates growth and bone mass. Journal of Clinical Investigation, 124(7), 2988-3002. https://doi.org/10.1172/JCI72606

Roman-Garcia, P, Quiros-Gonzalez, I, Mottram, L, Lieben, L, Sharan, K, Wangwiwatsin, A, Tubio, J, Lewis, K, Wilkinson, D, Santhanam, B, Sarper, N, Clare, S, Vassiliou, GS, Velagapudi, VR, Dougan, G & Yadav, VK 2014, 'Vitamin B₁₂-dependent taurine synthesis regulates growth and bone mass', Journal of Clinical Investigation, vol. 124, no. 7, pp. 2988-3002. https://doi.org/10.1172/JCI72606

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title = "Vitamin B12-dependent taurine synthesis regulates growth and bone mass",

abstract = "Both maternal and offspring-derived factors contribute to lifelong growth and bone mass accrual, although the specific role of maternal deficiencies in the growth and bone mass of offspring is poorly understood. In the present study, we have shown that vitamin B12 (B12) deficiency in a murine genetic model results in severe postweaning growth retardation and osteoporosis, and the severity and time of onset of this phenotype in the offspring depends on the maternal genotype. Using integrated physiological and metabolomic analysis, we determined that B12 deficiency in the offspring decreases liver taurine production and associates with abrogation of a growth hormone/insulin-like growth factor 1 (GH/IGF1) axis. Taurine increased GH-dependent IGF1 synthesis in the liver, which subsequently enhanced osteoblast function, and in B12-deficient offspring, oral administration of taurine rescued their growth retardation and osteoporosis phenotypes. These results identify B12 as an essential vitamin that positively regulates postweaning growth and bone formation through taurine synthesis and suggests potential therapies to increase bone mass.",

author = "Pablo Roman-Garcia and Isabel Quiros-Gonzalez and Lynda Mottram and Liesbet Lieben and Kunal Sharan and Arporn Wangwiwatsin and Jose Tubio and Kirsty Lewis and Debbie Wilkinson and Balaji Santhanam and Nazan Sarper and Simon Clare and Vassiliou, {George S.} and Velagapudi, {Vidya R.} and Gordon Dougan and Yadav, {Vijay K.}",

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AU - Quiros-Gonzalez, Isabel

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AU - Sharan, Kunal

AU - Wangwiwatsin, Arporn

AU - Tubio, Jose

AU - Lewis, Kirsty

AU - Wilkinson, Debbie

AU - Santhanam, Balaji

AU - Sarper, Nazan

AU - Clare, Simon

AU - Vassiliou, George S.

AU - Velagapudi, Vidya R.

AU - Dougan, Gordon

AU - Yadav, Vijay K.

PY - 2014/7/1

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N2 - Both maternal and offspring-derived factors contribute to lifelong growth and bone mass accrual, although the specific role of maternal deficiencies in the growth and bone mass of offspring is poorly understood. In the present study, we have shown that vitamin B12 (B12) deficiency in a murine genetic model results in severe postweaning growth retardation and osteoporosis, and the severity and time of onset of this phenotype in the offspring depends on the maternal genotype. Using integrated physiological and metabolomic analysis, we determined that B12 deficiency in the offspring decreases liver taurine production and associates with abrogation of a growth hormone/insulin-like growth factor 1 (GH/IGF1) axis. Taurine increased GH-dependent IGF1 synthesis in the liver, which subsequently enhanced osteoblast function, and in B12-deficient offspring, oral administration of taurine rescued their growth retardation and osteoporosis phenotypes. These results identify B12 as an essential vitamin that positively regulates postweaning growth and bone formation through taurine synthesis and suggests potential therapies to increase bone mass.

AB - Both maternal and offspring-derived factors contribute to lifelong growth and bone mass accrual, although the specific role of maternal deficiencies in the growth and bone mass of offspring is poorly understood. In the present study, we have shown that vitamin B12 (B12) deficiency in a murine genetic model results in severe postweaning growth retardation and osteoporosis, and the severity and time of onset of this phenotype in the offspring depends on the maternal genotype. Using integrated physiological and metabolomic analysis, we determined that B12 deficiency in the offspring decreases liver taurine production and associates with abrogation of a growth hormone/insulin-like growth factor 1 (GH/IGF1) axis. Taurine increased GH-dependent IGF1 synthesis in the liver, which subsequently enhanced osteoblast function, and in B12-deficient offspring, oral administration of taurine rescued their growth retardation and osteoporosis phenotypes. These results identify B12 as an essential vitamin that positively regulates postweaning growth and bone formation through taurine synthesis and suggests potential therapies to increase bone mass.

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Vitamin B₁₂-dependent taurine synthesis regulates growth and bone mass

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