Deletion at an 1q24 locus reveals a critical role of long noncoding RNA DNM3OS in skeletal development

Ting ting Yu; Qiu fan Xu; Si Yang Li; Hui jie Huang; Sarah Dugan; Lei Shao; Jennifer A. Roggenbuck; Xiao tong Liu; Huai ze Liu; Betsy A. Hirsch; Shen Yue; Chen Liu; Steven Y. Cheng

doi:10.1186/s13578-021-00559-8

Deletion at an 1q24 locus reveals a critical role of long noncoding RNA DNM3OS in skeletal development

Ting ting Yu, Qiu fan Xu, Si Yang Li, Hui jie Huang, Sarah Dugan, Lei Shao, Jennifer A. Roggenbuck, Xiao tong Liu, Huai ze Liu, Betsy A. Hirsch, Shen Yue, Chen Liu, Steven Y. Cheng

Laboratory Medicine and Pathology

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3 Scopus citations

Abstract

Background: Skeletal development and maintenance are complex processes known to be coordinated by multiple genetic and epigenetic signaling pathways. However, the role of long non-coding RNAs (lncRNAs), a class of crucial epigenetic regulatory molecules, has been under explored in skeletal biology. Results: Here we report a young patient with short stature, hypothalamic dysfunction and mild macrocephaly, who carries a maternally inherited 690 kb deletion at Chr.1q24.2 encompassing a noncoding RNA gene, DNM3OS, embedded on the opposite strand in an intron of the DYNAMIN 3 (DNM3) gene. We show that lncRNA DNM3OS sustains the proliferation of chondrocytes independent of two co-cistronic microRNAs miR-199a and miR-214. We further show that nerve growth factor (NGF), a known factor of chondrocyte growth, is a key target of DNM3OS-mediated control of chondrocyte proliferation. Conclusions: This work demonstrates that DNM3OS is essential for preventing premature differentiation of chondrocytes required for bone growth through endochondral ossification.

Original language	English (US)
Article number	47
Journal	Cell and Bioscience
Volume	11
Issue number	1
DOIs	https://doi.org/10.1186/s13578-021-00559-8
State	Published - Dec 2021

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Publisher Copyright:
© 2021, The Author(s).

Keywords

1q24
DNM3OS
Nerve growth factor
Skeletal abnormalities
lncRNA

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title = "Deletion at an 1q24 locus reveals a critical role of long noncoding RNA DNM3OS in skeletal development",

abstract = "Background: Skeletal development and maintenance are complex processes known to be coordinated by multiple genetic and epigenetic signaling pathways. However, the role of long non-coding RNAs (lncRNAs), a class of crucial epigenetic regulatory molecules, has been under explored in skeletal biology. Results: Here we report a young patient with short stature, hypothalamic dysfunction and mild macrocephaly, who carries a maternally inherited 690 kb deletion at Chr.1q24.2 encompassing a noncoding RNA gene, DNM3OS, embedded on the opposite strand in an intron of the DYNAMIN 3 (DNM3) gene. We show that lncRNA DNM3OS sustains the proliferation of chondrocytes independent of two co-cistronic microRNAs miR-199a and miR-214. We further show that nerve growth factor (NGF), a known factor of chondrocyte growth, is a key target of DNM3OS-mediated control of chondrocyte proliferation. Conclusions: This work demonstrates that DNM3OS is essential for preventing premature differentiation of chondrocytes required for bone growth through endochondral ossification.",

keywords = "1q24, DNM3OS, Nerve growth factor, Skeletal abnormalities, lncRNA",

author = "Yu, {Ting ting} and Xu, {Qiu fan} and Li, {Si Yang} and Huang, {Hui jie} and Sarah Dugan and Lei Shao and Roggenbuck, {Jennifer A.} and Liu, {Xiao tong} and Liu, {Huai ze} and Hirsch, {Betsy A.} and Shen Yue and Chen Liu and Cheng, {Steven Y.}",

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doi = "10.1186/s13578-021-00559-8",

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T1 - Deletion at an 1q24 locus reveals a critical role of long noncoding RNA DNM3OS in skeletal development

AU - Yu, Ting ting

AU - Xu, Qiu fan

AU - Li, Si Yang

AU - Huang, Hui jie

AU - Dugan, Sarah

AU - Shao, Lei

AU - Roggenbuck, Jennifer A.

AU - Liu, Xiao tong

AU - Liu, Huai ze

AU - Hirsch, Betsy A.

AU - Yue, Shen

AU - Liu, Chen

AU - Cheng, Steven Y.

PY - 2021/12

Y1 - 2021/12

N2 - Background: Skeletal development and maintenance are complex processes known to be coordinated by multiple genetic and epigenetic signaling pathways. However, the role of long non-coding RNAs (lncRNAs), a class of crucial epigenetic regulatory molecules, has been under explored in skeletal biology. Results: Here we report a young patient with short stature, hypothalamic dysfunction and mild macrocephaly, who carries a maternally inherited 690 kb deletion at Chr.1q24.2 encompassing a noncoding RNA gene, DNM3OS, embedded on the opposite strand in an intron of the DYNAMIN 3 (DNM3) gene. We show that lncRNA DNM3OS sustains the proliferation of chondrocytes independent of two co-cistronic microRNAs miR-199a and miR-214. We further show that nerve growth factor (NGF), a known factor of chondrocyte growth, is a key target of DNM3OS-mediated control of chondrocyte proliferation. Conclusions: This work demonstrates that DNM3OS is essential for preventing premature differentiation of chondrocytes required for bone growth through endochondral ossification.

AB - Background: Skeletal development and maintenance are complex processes known to be coordinated by multiple genetic and epigenetic signaling pathways. However, the role of long non-coding RNAs (lncRNAs), a class of crucial epigenetic regulatory molecules, has been under explored in skeletal biology. Results: Here we report a young patient with short stature, hypothalamic dysfunction and mild macrocephaly, who carries a maternally inherited 690 kb deletion at Chr.1q24.2 encompassing a noncoding RNA gene, DNM3OS, embedded on the opposite strand in an intron of the DYNAMIN 3 (DNM3) gene. We show that lncRNA DNM3OS sustains the proliferation of chondrocytes independent of two co-cistronic microRNAs miR-199a and miR-214. We further show that nerve growth factor (NGF), a known factor of chondrocyte growth, is a key target of DNM3OS-mediated control of chondrocyte proliferation. Conclusions: This work demonstrates that DNM3OS is essential for preventing premature differentiation of chondrocytes required for bone growth through endochondral ossification.

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Deletion at an 1q24 locus reveals a critical role of long noncoding RNA DNM3OS in skeletal development

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