Nf1-Dependent Tumors Require a Microenvironment Containing Nf1+/-- and c-kit-Dependent Bone Marrow

Feng Chun Yang; David A. Ingram; Shi Chen; Yuan Zhu; Jin Yuan; Xiaohong Li; Xianlin Yang; Scott Knowles; Whitney Horn; Yan Li; Shaobo Zhang; Yanzhu Yang; Saeed T. Vakili; Menggang Yu; Dennis Burns; Kent Robertson; Gary Hutchins; Luis F. Parada; D. Wade Clapp

doi:10.1016/j.cell.2008.08.041

Nf1-Dependent Tumors Require a Microenvironment Containing Nf1^+/-- and c-kit-Dependent Bone Marrow

Feng Chun Yang, David A. Ingram, Shi Chen, Yuan Zhu, Jin Yuan, Xiaohong Li, Xianlin Yang, Scott Knowles, Whitney Horn, Yan Li, Shaobo Zhang, Yanzhu Yang, Saeed T. Vakili, Menggang Yu, Dennis Burns, Kent Robertson, Gary Hutchins, Luis F. Parada, D. Wade Clapp

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

307 Scopus citations

Abstract

Interactions between tumorigenic cells and their surrounding microenvironment are critical for tumor progression yet remain incompletely understood. Germline mutations in the NF1 tumor suppressor gene cause neurofibromatosis type 1 (NF1), a common genetic disorder characterized by complex tumors called neurofibromas. Genetic studies indicate that biallelic loss of Nf1 is required in the tumorigenic cell of origin in the embryonic Schwann cell lineage. However, in the physiologic state, Schwann cell loss of heterozygosity is not sufficient for neurofibroma formation and Nf1 haploinsufficiency in at least one additional nonneoplastic lineage is required for tumor progression. Here, we establish that Nf1 heterozygosity of bone marrow-derived cells in the tumor microenvironment is sufficient to allow neurofibroma progression in the context of Schwann cell Nf1 deficiency. Further, genetic or pharmacologic attenuation of c-kit signaling in Nf1^+/- hematopoietic cells diminishes neurofibroma initiation and progression. Finally, these studies implicate mast cells as critical mediators of tumor initiation.

Original language	English (US)
Pages (from-to)	437-448
Number of pages	12
Journal	Cell
Volume	135
Issue number	3
DOIs	https://doi.org/10.1016/j.cell.2008.08.041
State	Published - Oct 31 2008

Keywords

CELLCYCLE
HUMDISEASE

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.1016/j.cell.2008.08.041

Cite this

Yang, F. C., Ingram, D. A., Chen, S., Zhu, Y., Yuan, J., Li, X., Yang, X., Knowles, S., Horn, W., Li, Y., Zhang, S., Yang, Y., Vakili, S. T., Yu, M., Burns, D., Robertson, K., Hutchins, G., Parada, L. F., & Clapp, D. W. (2008). Nf1-Dependent Tumors Require a Microenvironment Containing Nf1^+/-- and c-kit-Dependent Bone Marrow. Cell, 135(3), 437-448. https://doi.org/10.1016/j.cell.2008.08.041

Yang, FC, Ingram, DA, Chen, S, Zhu, Y, Yuan, J, Li, X, Yang, X, Knowles, S, Horn, W, Li, Y, Zhang, S, Yang, Y, Vakili, ST, Yu, M, Burns, D, Robertson, K, Hutchins, G, Parada, LF & Clapp, DW 2008, 'Nf1-Dependent Tumors Require a Microenvironment Containing Nf1^+/-- and c-kit-Dependent Bone Marrow', Cell, vol. 135, no. 3, pp. 437-448. https://doi.org/10.1016/j.cell.2008.08.041

@article{d99cd1c00d734ec89093b6c5052a7ce2,

title = "Nf1-Dependent Tumors Require a Microenvironment Containing Nf1+/-- and c-kit-Dependent Bone Marrow",

abstract = "Interactions between tumorigenic cells and their surrounding microenvironment are critical for tumor progression yet remain incompletely understood. Germline mutations in the NF1 tumor suppressor gene cause neurofibromatosis type 1 (NF1), a common genetic disorder characterized by complex tumors called neurofibromas. Genetic studies indicate that biallelic loss of Nf1 is required in the tumorigenic cell of origin in the embryonic Schwann cell lineage. However, in the physiologic state, Schwann cell loss of heterozygosity is not sufficient for neurofibroma formation and Nf1 haploinsufficiency in at least one additional nonneoplastic lineage is required for tumor progression. Here, we establish that Nf1 heterozygosity of bone marrow-derived cells in the tumor microenvironment is sufficient to allow neurofibroma progression in the context of Schwann cell Nf1 deficiency. Further, genetic or pharmacologic attenuation of c-kit signaling in Nf1+/- hematopoietic cells diminishes neurofibroma initiation and progression. Finally, these studies implicate mast cells as critical mediators of tumor initiation.",

keywords = "CELLCYCLE, HUMDISEASE",

author = "Yang, {Feng Chun} and Ingram, {David A.} and Shi Chen and Yuan Zhu and Jin Yuan and Xiaohong Li and Xianlin Yang and Scott Knowles and Whitney Horn and Yan Li and Shaobo Zhang and Yanzhu Yang and Vakili, {Saeed T.} and Menggang Yu and Dennis Burns and Kent Robertson and Gary Hutchins and Parada, {Luis F.} and Clapp, {D. Wade}",

note = "Funding Information: This work was supported by the Department of Defense (NF020026) to D.W.C. and L.F.P., a P50 Center of Excellence in Neurofibromatosis P50 NS 052606 (L.F.P., D.W.C., F.C.Y., D.A.I., and G.H.) and R01 CA74177 to D.W.C. L.F.P. is an American Cancer Society Professor and also acknowledges support from the NCI-MMHC. Novartis supplied imatinib mesylate to D.W.C. for these studies. The work was also supported by the Anna Fuller Foundation. ",

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doi = "10.1016/j.cell.2008.08.041",

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AU - Yang, Feng Chun

AU - Ingram, David A.

AU - Chen, Shi

AU - Zhu, Yuan

AU - Yuan, Jin

AU - Li, Xiaohong

AU - Yang, Xianlin

AU - Knowles, Scott

AU - Horn, Whitney

AU - Li, Yan

AU - Zhang, Shaobo

AU - Yang, Yanzhu

AU - Vakili, Saeed T.

AU - Yu, Menggang

AU - Burns, Dennis

AU - Robertson, Kent

AU - Hutchins, Gary

AU - Parada, Luis F.

AU - Clapp, D. Wade

N1 - Funding Information: This work was supported by the Department of Defense (NF020026) to D.W.C. and L.F.P., a P50 Center of Excellence in Neurofibromatosis P50 NS 052606 (L.F.P., D.W.C., F.C.Y., D.A.I., and G.H.) and R01 CA74177 to D.W.C. L.F.P. is an American Cancer Society Professor and also acknowledges support from the NCI-MMHC. Novartis supplied imatinib mesylate to D.W.C. for these studies. The work was also supported by the Anna Fuller Foundation.

PY - 2008/10/31

Y1 - 2008/10/31

N2 - Interactions between tumorigenic cells and their surrounding microenvironment are critical for tumor progression yet remain incompletely understood. Germline mutations in the NF1 tumor suppressor gene cause neurofibromatosis type 1 (NF1), a common genetic disorder characterized by complex tumors called neurofibromas. Genetic studies indicate that biallelic loss of Nf1 is required in the tumorigenic cell of origin in the embryonic Schwann cell lineage. However, in the physiologic state, Schwann cell loss of heterozygosity is not sufficient for neurofibroma formation and Nf1 haploinsufficiency in at least one additional nonneoplastic lineage is required for tumor progression. Here, we establish that Nf1 heterozygosity of bone marrow-derived cells in the tumor microenvironment is sufficient to allow neurofibroma progression in the context of Schwann cell Nf1 deficiency. Further, genetic or pharmacologic attenuation of c-kit signaling in Nf1+/- hematopoietic cells diminishes neurofibroma initiation and progression. Finally, these studies implicate mast cells as critical mediators of tumor initiation.

AB - Interactions between tumorigenic cells and their surrounding microenvironment are critical for tumor progression yet remain incompletely understood. Germline mutations in the NF1 tumor suppressor gene cause neurofibromatosis type 1 (NF1), a common genetic disorder characterized by complex tumors called neurofibromas. Genetic studies indicate that biallelic loss of Nf1 is required in the tumorigenic cell of origin in the embryonic Schwann cell lineage. However, in the physiologic state, Schwann cell loss of heterozygosity is not sufficient for neurofibroma formation and Nf1 haploinsufficiency in at least one additional nonneoplastic lineage is required for tumor progression. Here, we establish that Nf1 heterozygosity of bone marrow-derived cells in the tumor microenvironment is sufficient to allow neurofibroma progression in the context of Schwann cell Nf1 deficiency. Further, genetic or pharmacologic attenuation of c-kit signaling in Nf1+/- hematopoietic cells diminishes neurofibroma initiation and progression. Finally, these studies implicate mast cells as critical mediators of tumor initiation.

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KW - HUMDISEASE

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