Latexin Inactivation Enhances Survival and Long-Term Engraftment of Hematopoietic Stem Cells and Expands the Entire Hematopoietic System in Mice

Yi Liu; Cuiping Zhang; Zhenyu Li; Chi Wang; Jianhang Jia; Tianyan Gao; Gerhard Hildebrandt; Daohong Zhou; Subbarao Bondada; Peng Ji; Daret St. Clair; Jinze Liu; Changguo Zhan; Hartmut Geiger; Shuxia Wang; Ying Liang

doi:10.1016/j.stemcr.2017.02.009

Latexin Inactivation Enhances Survival and Long-Term Engraftment of Hematopoietic Stem Cells and Expands the Entire Hematopoietic System in Mice

Yi Liu, Cuiping Zhang, Zhenyu Li, Chi Wang, Jianhang Jia, Tianyan Gao, Gerhard Hildebrandt, Daohong Zhou, Subbarao Bondada, Peng Ji, Daret St. Clair, Jinze Liu, Changguo Zhan, Hartmut Geiger, Shuxia Wang, Ying Liang

Producción científica: Article › revisión exhaustiva

21 Citas (Scopus)

Resumen

Natural genetic diversity offers an important yet largely untapped resource to decipher the molecular mechanisms regulating hematopoietic stem cell (HSC) function. Latexin (Lxn) is a negative stem cell regulatory gene identified on the basis of genetic diversity. By using an Lxn knockout mouse model, we found that Lxn inactivation in vivo led to the physiological expansion of the entire hematopoietic hierarchy. Loss of Lxn enhanced the competitive repopulation capacity and survival of HSCs in a cell-intrinsic manner. Gene profiling of Lxn-null HSCs showed altered expression of genes enriched in cell-matrix and cell-cell interactions. Thrombospondin 1 (Thbs1) was a potential downstream target with a dramatic downregulation in Lxn-null HSCs. Enforced expression of Thbs1 restored the Lxn inactivation-mediated HSC phenotypes. This study reveals that Lxn plays an important role in the maintenance of homeostatic hematopoiesis, and it may lead to development of safe and effective approaches to manipulate HSCs for clinical benefit.

Idioma original	English (US)
Páginas (desde-hasta)	991-1004
Número de páginas	14
Publicación	Stem Cell Reports
Volumen	8
N.º	4
DOI	https://doi.org/10.1016/j.stemcr.2017.02.009
Estado	Published - abr 11 2017
Publicado de forma externa	Sí

ASJC Scopus subject areas

Genetics
Biochemistry
Cell Biology
Developmental Biology

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10.1016/j.stemcr.2017.02.009

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Liu, Y., Zhang, C., Li, Z., Wang, C., Jia, J., Gao, T., Hildebrandt, G., Zhou, D., Bondada, S., Ji, P., St. Clair, D., Liu, J., Zhan, C., Geiger, H., Wang, S., & Liang, Y. (2017). Latexin Inactivation Enhances Survival and Long-Term Engraftment of Hematopoietic Stem Cells and Expands the Entire Hematopoietic System in Mice. Stem Cell Reports, 8(4), 991-1004. https://doi.org/10.1016/j.stemcr.2017.02.009

Liu, Y, Zhang, C, Li, Z, Wang, C, Jia, J, Gao, T, Hildebrandt, G, Zhou, D, Bondada, S, Ji, P, St. Clair, D, Liu, J, Zhan, C, Geiger, H, Wang, S & Liang, Y 2017, 'Latexin Inactivation Enhances Survival and Long-Term Engraftment of Hematopoietic Stem Cells and Expands the Entire Hematopoietic System in Mice', Stem Cell Reports, vol. 8, n.º 4, pp. 991-1004. https://doi.org/10.1016/j.stemcr.2017.02.009

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abstract = "Natural genetic diversity offers an important yet largely untapped resource to decipher the molecular mechanisms regulating hematopoietic stem cell (HSC) function. Latexin (Lxn) is a negative stem cell regulatory gene identified on the basis of genetic diversity. By using an Lxn knockout mouse model, we found that Lxn inactivation in vivo led to the physiological expansion of the entire hematopoietic hierarchy. Loss of Lxn enhanced the competitive repopulation capacity and survival of HSCs in a cell-intrinsic manner. Gene profiling of Lxn-null HSCs showed altered expression of genes enriched in cell-matrix and cell-cell interactions. Thrombospondin 1 (Thbs1) was a potential downstream target with a dramatic downregulation in Lxn-null HSCs. Enforced expression of Thbs1 restored the Lxn inactivation-mediated HSC phenotypes. This study reveals that Lxn plays an important role in the maintenance of homeostatic hematopoiesis, and it may lead to development of safe and effective approaches to manipulate HSCs for clinical benefit.",

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AU - Zhang, Cuiping

AU - Li, Zhenyu

AU - Wang, Chi

AU - Jia, Jianhang

AU - Gao, Tianyan

AU - Hildebrandt, Gerhard

AU - Zhou, Daohong

AU - Bondada, Subbarao

AU - Ji, Peng

AU - St. Clair, Daret

AU - Liu, Jinze

AU - Zhan, Changguo

AU - Geiger, Hartmut

AU - Wang, Shuxia

AU - Liang, Ying

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N2 - Natural genetic diversity offers an important yet largely untapped resource to decipher the molecular mechanisms regulating hematopoietic stem cell (HSC) function. Latexin (Lxn) is a negative stem cell regulatory gene identified on the basis of genetic diversity. By using an Lxn knockout mouse model, we found that Lxn inactivation in vivo led to the physiological expansion of the entire hematopoietic hierarchy. Loss of Lxn enhanced the competitive repopulation capacity and survival of HSCs in a cell-intrinsic manner. Gene profiling of Lxn-null HSCs showed altered expression of genes enriched in cell-matrix and cell-cell interactions. Thrombospondin 1 (Thbs1) was a potential downstream target with a dramatic downregulation in Lxn-null HSCs. Enforced expression of Thbs1 restored the Lxn inactivation-mediated HSC phenotypes. This study reveals that Lxn plays an important role in the maintenance of homeostatic hematopoiesis, and it may lead to development of safe and effective approaches to manipulate HSCs for clinical benefit.

AB - Natural genetic diversity offers an important yet largely untapped resource to decipher the molecular mechanisms regulating hematopoietic stem cell (HSC) function. Latexin (Lxn) is a negative stem cell regulatory gene identified on the basis of genetic diversity. By using an Lxn knockout mouse model, we found that Lxn inactivation in vivo led to the physiological expansion of the entire hematopoietic hierarchy. Loss of Lxn enhanced the competitive repopulation capacity and survival of HSCs in a cell-intrinsic manner. Gene profiling of Lxn-null HSCs showed altered expression of genes enriched in cell-matrix and cell-cell interactions. Thrombospondin 1 (Thbs1) was a potential downstream target with a dramatic downregulation in Lxn-null HSCs. Enforced expression of Thbs1 restored the Lxn inactivation-mediated HSC phenotypes. This study reveals that Lxn plays an important role in the maintenance of homeostatic hematopoiesis, and it may lead to development of safe and effective approaches to manipulate HSCs for clinical benefit.

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