Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis

Steven D. Rhodes; Hao Yang; Ruizhi Dong; Keshav Menon; Yongzheng He; Zhaomin Li; Shi Chen; Karl W. Staser; Li Jiang; Xiaohua Wu; Xianlin Yang; Xianghong Peng; Khalid S. Mohammad; Theresa A. Guise; Mingjiang Xu; Feng Chun Yang

doi:10.1002/jbmr.2538

Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis

Steven D. Rhodes
, Hao Yang
, Ruizhi Dong
, Keshav Menon
, Yongzheng He
, Zhaomin Li
, Shi Chen
, Karl W. Staser
, Li Jiang
, Xiaohua Wu
, Xianlin Yang
, Xianghong Peng
, Khalid S. Mohammad
, Theresa A. Guise
, Mingjiang Xu
, Feng Chun Yang

Producción científica: Article › revisión exhaustiva

6 Citas (Scopus)

Resumen

Although nullizygous loss of NF1 leads to myeloid malignancies, haploinsufficient loss of NF1 (Nf1) has been shown to contribute to osteopenia and osteoporosis which occurs in approximately 50% of neurofibromatosis type 1 (NF1) patients. Bone marrow mononuclear cells of haploinsufficient NF1 patients and Nf1^+/- mice exhibit increased osteoclastogenesis and accelerated bone turnover; however, the culprit hematopoietic lineages responsible for perpetuating these osteolytic manifestations have yet to be elucidated. Here we demonstrate that conditional inactivation of a single Nf1 allele within the myeloid progenitor cell population (Nf1-LysM) is necessary and sufficient to promote multiple osteoclast gains-in-function, resulting in enhanced osteoclastogenesis and accelerated osteoclast bone lytic activity in response to proresorptive challenge in vivo. Surprisingly, mice conditionally Nf1 heterozygous in mature, terminally differentiated osteoclasts (Nf1-Ctsk) do not exhibit any of these skeletal phenotypes, indicating a critical requirement for Nf1 haploinsufficiency at a more primitive/progenitor stage of myeloid development in perpetuating osteolytic activity. We further identified p21Ras-dependent hyperphosphorylation of Pu.1 within the nucleus of Nf1 haploinsufficient myelomonocytic osteoclast precursors, providing a novel therapeutic target for the potential treatment of NF1 associated osteolytic manifestations.

Idioma original	English (US)
Páginas (desde-hasta)	1840-1851
Número de páginas	12
Publicación	Journal of Bone and Mineral Research
Volumen	30
N.º	10
DOI	https://doi.org/10.1002/jbmr.2538
Estado	Published - oct 1 2015
Publicado de forma externa	Sí

ASJC Scopus subject areas

Endocrinology, Diabetes and Metabolism
Orthopedics and Sports Medicine

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10.1002/jbmr.2538

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Rhodes, S. D., Yang, H., Dong, R., Menon, K., He, Y., Li, Z., Chen, S., Staser, K. W., Jiang, L., Wu, X., Yang, X., Peng, X., Mohammad, K. S., Guise, T. A., Xu, M., & Yang, F. C. (2015). Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis. Journal of Bone and Mineral Research, 30(10), 1840-1851. https://doi.org/10.1002/jbmr.2538

Rhodes, SD, Yang, H, Dong, R, Menon, K, He, Y, Li, Z, Chen, S, Staser, KW, Jiang, L, Wu, X, Yang, X, Peng, X, Mohammad, KS, Guise, TA, Xu, M & Yang, FC 2015, 'Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis', Journal of Bone and Mineral Research, vol. 30, n.º 10, pp. 1840-1851. https://doi.org/10.1002/jbmr.2538

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title = "Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis",

abstract = "Although nullizygous loss of NF1 leads to myeloid malignancies, haploinsufficient loss of NF1 (Nf1) has been shown to contribute to osteopenia and osteoporosis which occurs in approximately 50\% of neurofibromatosis type 1 (NF1) patients. Bone marrow mononuclear cells of haploinsufficient NF1 patients and Nf1+/- mice exhibit increased osteoclastogenesis and accelerated bone turnover; however, the culprit hematopoietic lineages responsible for perpetuating these osteolytic manifestations have yet to be elucidated. Here we demonstrate that conditional inactivation of a single Nf1 allele within the myeloid progenitor cell population (Nf1-LysM) is necessary and sufficient to promote multiple osteoclast gains-in-function, resulting in enhanced osteoclastogenesis and accelerated osteoclast bone lytic activity in response to proresorptive challenge in vivo. Surprisingly, mice conditionally Nf1 heterozygous in mature, terminally differentiated osteoclasts (Nf1-Ctsk) do not exhibit any of these skeletal phenotypes, indicating a critical requirement for Nf1 haploinsufficiency at a more primitive/progenitor stage of myeloid development in perpetuating osteolytic activity. We further identified p21Ras-dependent hyperphosphorylation of Pu.1 within the nucleus of Nf1 haploinsufficient myelomonocytic osteoclast precursors, providing a novel therapeutic target for the potential treatment of NF1 associated osteolytic manifestations.",

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AU - Yang, Hao

AU - Dong, Ruizhi

AU - Menon, Keshav

AU - He, Yongzheng

AU - Li, Zhaomin

AU - Chen, Shi

AU - Staser, Karl W.

AU - Jiang, Li

AU - Wu, Xiaohua

AU - Yang, Xianlin

AU - Peng, Xianghong

AU - Mohammad, Khalid S.

AU - Guise, Theresa A.

AU - Xu, Mingjiang

AU - Yang, Feng Chun

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AB - Although nullizygous loss of NF1 leads to myeloid malignancies, haploinsufficient loss of NF1 (Nf1) has been shown to contribute to osteopenia and osteoporosis which occurs in approximately 50% of neurofibromatosis type 1 (NF1) patients. Bone marrow mononuclear cells of haploinsufficient NF1 patients and Nf1+/- mice exhibit increased osteoclastogenesis and accelerated bone turnover; however, the culprit hematopoietic lineages responsible for perpetuating these osteolytic manifestations have yet to be elucidated. Here we demonstrate that conditional inactivation of a single Nf1 allele within the myeloid progenitor cell population (Nf1-LysM) is necessary and sufficient to promote multiple osteoclast gains-in-function, resulting in enhanced osteoclastogenesis and accelerated osteoclast bone lytic activity in response to proresorptive challenge in vivo. Surprisingly, mice conditionally Nf1 heterozygous in mature, terminally differentiated osteoclasts (Nf1-Ctsk) do not exhibit any of these skeletal phenotypes, indicating a critical requirement for Nf1 haploinsufficiency at a more primitive/progenitor stage of myeloid development in perpetuating osteolytic activity. We further identified p21Ras-dependent hyperphosphorylation of Pu.1 within the nucleus of Nf1 haploinsufficient myelomonocytic osteoclast precursors, providing a novel therapeutic target for the potential treatment of NF1 associated osteolytic manifestations.

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Nf1 haploinsufficiency alters myeloid lineage commitment and function, leading to deranged skeletal homeostasis

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