Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia

Afonso R.M. Almeida; João L. Neto; Ana Cachucho; Mayara Euzébio; Xiangyu Meng; Rathana Kim; Marta B. Fernandes; Beatriz Raposo; Mariana L. Oliveira; Daniel Ribeiro; Rita Fragoso; Priscila P. Zenatti; Tiago Soares; Mafalda R. de Matos; Juliana Ronchi Corrêa; Mafalda Duque; Kathryn G. Roberts; Zhaohui Gu; Chunxu Qu; Clara Pereira; Susan Pyne; Nigel J. Pyne; Vasco M. Barreto; Isabelle Bernard-Pierrot; Emannuelle Clappier; Charles G. Mullighan; Ana R. Grosso; J. Andrés Yunes; João T. Barata

doi:10.1038/s41467-021-27197-5

Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia

Afonso R.M. Almeida
, João L. Neto
, Ana Cachucho
, Mayara Euzébio
, Xiangyu Meng
, Rathana Kim
, Marta B. Fernandes
, Beatriz Raposo
, Mariana L. Oliveira
, Daniel Ribeiro
, Rita Fragoso
, Priscila P. Zenatti
, Tiago Soares
, Mafalda R. de Matos
, Juliana Ronchi Corrêa
, Mafalda Duque
, Kathryn G. Roberts
, Zhaohui Gu
, Chunxu Qu
, Clara Pereira

Susan Pyne, Nigel J. Pyne, Vasco M. Barreto, Isabelle Bernard-Pierrot, Emannuelle Clappier, Charles G. Mullighan, Ana R. Grosso, J. Andrés Yunes, João T. Barata

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Resumo

Interleukin-7 receptor α (encoded by IL7R) is essential for lymphoid development. Whether acute lymphoblastic leukemia (ALL)-related IL7R gain-of-function mutations can trigger leukemogenesis remains unclear. Here, we demonstrate that lymphoid-restricted mutant IL7R, expressed at physiological levels in conditional knock-in mice, establishes a pre-leukemic stage in which B-cell precursors display self-renewal ability, initiating leukemia resembling PAX5 P80R or Ph-like human B-ALL. Full transformation associates with transcriptional upregulation of oncogenes such as Myc or Bcl2, downregulation of tumor suppressors such as Ikzf1 or Arid2, and major IL-7R signaling upregulation (involving JAK/STAT5 and PI3K/mTOR), required for leukemia cell viability. Accordingly, maximal signaling drives full penetrance and early leukemia onset in homozygous IL7R mutant animals. Notably, we identify 2 transcriptional subgroups in mouse and human Ph-like ALL, and show that dactolisib and sphingosine-kinase inhibitors are potential treatment avenues for IL-7R-related cases. Our model, a resource to explore the pathophysiology and therapeutic vulnerabilities of B-ALL, demonstrates that IL7R can initiate this malignancy.

Idioma original	???core.languages.en_GB???
Número do artigo	7268
Revista	Nature Communications
Volume	12
Número de emissão	1
DOIs	https://doi.org/10.1038/s41467-021-27197-5
Estado da publicação	???researchoutput.status.published??? - dez. 2021
Publicado externamente	Sim

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Almeida, A. R. M., Neto, J. L., Cachucho, A., Euzébio, M., Meng, X., Kim, R., Fernandes, M. B., Raposo, B., Oliveira, M. L., Ribeiro, D., Fragoso, R., Zenatti, P. P., Soares, T., de Matos, M. R., Corrêa, J. R., Duque, M., Roberts, K. G., Gu, Z., Qu, C., ... Barata, J. T. (2021). Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia. Nature Communications, 12(1), Artigo 7268. https://doi.org/10.1038/s41467-021-27197-5

@article{d913f179b1cb487ca5fcfffcdd679388,

title = "Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia",

abstract = "Interleukin-7 receptor α (encoded by IL7R) is essential for lymphoid development. Whether acute lymphoblastic leukemia (ALL)-related IL7R gain-of-function mutations can trigger leukemogenesis remains unclear. Here, we demonstrate that lymphoid-restricted mutant IL7R, expressed at physiological levels in conditional knock-in mice, establishes a pre-leukemic stage in which B-cell precursors display self-renewal ability, initiating leukemia resembling PAX5 P80R or Ph-like human B-ALL. Full transformation associates with transcriptional upregulation of oncogenes such as Myc or Bcl2, downregulation of tumor suppressors such as Ikzf1 or Arid2, and major IL-7R signaling upregulation (involving JAK/STAT5 and PI3K/mTOR), required for leukemia cell viability. Accordingly, maximal signaling drives full penetrance and early leukemia onset in homozygous IL7R mutant animals. Notably, we identify 2 transcriptional subgroups in mouse and human Ph-like ALL, and show that dactolisib and sphingosine-kinase inhibitors are potential treatment avenues for IL-7R-related cases. Our model, a resource to explore the pathophysiology and therapeutic vulnerabilities of B-ALL, demonstrates that IL7R can initiate this malignancy.",

author = "Almeida, \{Afonso R.M.\} and Neto, \{Jo{\~a}o L.\} and Ana Cachucho and Mayara Euz{\'e}bio and Xiangyu Meng and Rathana Kim and Fernandes, \{Marta B.\} and Beatriz Raposo and Oliveira, \{Mariana L.\} and Daniel Ribeiro and Rita Fragoso and Zenatti, \{Priscila P.\} and Tiago Soares and \{de Matos\}, \{Mafalda R.\} and Corr{\^e}a, \{Juliana Ronchi\} and Mafalda Duque and Roberts, \{Kathryn G.\} and Zhaohui Gu and Chunxu Qu and Clara Pereira and Susan Pyne and Pyne, \{Nigel J.\} and Barreto, \{Vasco M.\} and Isabelle Bernard-Pierrot and Emannuelle Clappier and Mullighan, \{Charles G.\} and Grosso, \{Ana R.\} and Yunes, \{J. Andr{\'e}s\} and Barata, \{Jo{\~a}o T.\}",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = dec,

doi = "10.1038/s41467-021-27197-5",

language = "English",

volume = "12",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Research",

number = "1",

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Almeida, ARM, Neto, JL, Cachucho, A, Euzébio, M, Meng, X, Kim, R, Fernandes, MB, Raposo, B, Oliveira, ML, Ribeiro, D, Fragoso, R, Zenatti, PP, Soares, T, de Matos, MR, Corrêa, JR, Duque, M, Roberts, KG, Gu, Z, Qu, C, Pereira, C, Pyne, S, Pyne, NJ, Barreto, VM, Bernard-Pierrot, I, Clappier, E, Mullighan, CG, Grosso, AR, Yunes, JA & Barata, JT 2021, 'Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia', Nature Communications, vol. 12, n.º 1, 7268. https://doi.org/10.1038/s41467-021-27197-5

TY - JOUR

T1 - Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia

AU - Almeida, Afonso R.M.

AU - Neto, João L.

AU - Cachucho, Ana

AU - Euzébio, Mayara

AU - Meng, Xiangyu

AU - Kim, Rathana

AU - Fernandes, Marta B.

AU - Raposo, Beatriz

AU - Oliveira, Mariana L.

AU - Ribeiro, Daniel

AU - Fragoso, Rita

AU - Zenatti, Priscila P.

AU - Soares, Tiago

AU - de Matos, Mafalda R.

AU - Corrêa, Juliana Ronchi

AU - Duque, Mafalda

AU - Roberts, Kathryn G.

AU - Gu, Zhaohui

AU - Qu, Chunxu

AU - Pereira, Clara

AU - Pyne, Susan

AU - Pyne, Nigel J.

AU - Barreto, Vasco M.

AU - Bernard-Pierrot, Isabelle

AU - Clappier, Emannuelle

AU - Mullighan, Charles G.

AU - Grosso, Ana R.

AU - Yunes, J. Andrés

AU - Barata, João T.

PY - 2021/12

Y1 - 2021/12

N2 - Interleukin-7 receptor α (encoded by IL7R) is essential for lymphoid development. Whether acute lymphoblastic leukemia (ALL)-related IL7R gain-of-function mutations can trigger leukemogenesis remains unclear. Here, we demonstrate that lymphoid-restricted mutant IL7R, expressed at physiological levels in conditional knock-in mice, establishes a pre-leukemic stage in which B-cell precursors display self-renewal ability, initiating leukemia resembling PAX5 P80R or Ph-like human B-ALL. Full transformation associates with transcriptional upregulation of oncogenes such as Myc or Bcl2, downregulation of tumor suppressors such as Ikzf1 or Arid2, and major IL-7R signaling upregulation (involving JAK/STAT5 and PI3K/mTOR), required for leukemia cell viability. Accordingly, maximal signaling drives full penetrance and early leukemia onset in homozygous IL7R mutant animals. Notably, we identify 2 transcriptional subgroups in mouse and human Ph-like ALL, and show that dactolisib and sphingosine-kinase inhibitors are potential treatment avenues for IL-7R-related cases. Our model, a resource to explore the pathophysiology and therapeutic vulnerabilities of B-ALL, demonstrates that IL7R can initiate this malignancy.

AB - Interleukin-7 receptor α (encoded by IL7R) is essential for lymphoid development. Whether acute lymphoblastic leukemia (ALL)-related IL7R gain-of-function mutations can trigger leukemogenesis remains unclear. Here, we demonstrate that lymphoid-restricted mutant IL7R, expressed at physiological levels in conditional knock-in mice, establishes a pre-leukemic stage in which B-cell precursors display self-renewal ability, initiating leukemia resembling PAX5 P80R or Ph-like human B-ALL. Full transformation associates with transcriptional upregulation of oncogenes such as Myc or Bcl2, downregulation of tumor suppressors such as Ikzf1 or Arid2, and major IL-7R signaling upregulation (involving JAK/STAT5 and PI3K/mTOR), required for leukemia cell viability. Accordingly, maximal signaling drives full penetrance and early leukemia onset in homozygous IL7R mutant animals. Notably, we identify 2 transcriptional subgroups in mouse and human Ph-like ALL, and show that dactolisib and sphingosine-kinase inhibitors are potential treatment avenues for IL-7R-related cases. Our model, a resource to explore the pathophysiology and therapeutic vulnerabilities of B-ALL, demonstrates that IL7R can initiate this malignancy.

UR - https://www.scopus.com/pages/publications/85121306348

U2 - 10.1038/s41467-021-27197-5

DO - 10.1038/s41467-021-27197-5

M3 - Article

C2 - 34907175

AN - SCOPUS:85121306348

SN - 2041-1723

VL - 12

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 7268

ER -

Interleukin-7 receptor α mutational activation can initiate precursor B-cell acute lymphoblastic leukemia

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