Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency

Alvaro Muñoz-López; Damià Romero-Moya; Cristina Prieto; Verónica Ramos-Mejía; Antonio Agraz-Doblas; Ignacio Varela; Marcus Buschbeck; Anna Palau; Xonia Carvajal-Vergara; Alessandra Giorgetti; Anthony Ford; Majlinda Lako; Isabel Granada; Neus Ruiz-Xivillé; Sandra Rodríguez-Perales; Raul Torres-Ruíz; Ronald W. Stam; Jose Luis Fuster; Mario F. Fraga; Mahito Nakanishi; Gianni Cazzaniga; Michela Bardini; Isabel Cobo; Gustavo F. Bayon; Agustin F. Fernandez; Clara Bueno; Pablo Menendez

doi:10.1016/j.stemcr.2016.08.013

Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency

Alvaro Muñoz-López, Damià Romero-Moya, Cristina Prieto, Verónica Ramos-Mejía, Antonio Agraz-Doblas, Ignacio Varela, Marcus Buschbeck, Anna Palau, Xonia Carvajal-Vergara, Alessandra Giorgetti, Anthony Ford, Majlinda Lako, Isabel Granada, Neus Ruiz-Xivillé, Sandra Rodríguez-Perales, Raul Torres-Ruíz, Ronald W. Stam, Jose Luis Fuster, Mario F. Fraga, Mahito NakanishiGianni Cazzaniga, Michela Bardini, Isabel Cobo, Gustavo F. Bayon, Agustin F. Fernandez, Clara Bueno, Pablo Menendez

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

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Induced pluripotent stem cells (iPSCs) are a powerful tool for disease modeling. They are routinely generated from healthy donors and patients from multiple cell types at different developmental stages. However, reprogramming leukemias is an extremely inefficient process. Few studies generated iPSCs from primary chronic myeloid leukemias, but iPSC generation from acute myeloid or lymphoid leukemias (ALL) has not been achieved. We attempted to generate iPSCs from different subtypes of B-ALL to address the developmental impact of leukemic fusion genes. OKSM(L)-expressing mono/polycistronic-, retroviral/lentiviral/episomal-, and Sendai virus vector-based reprogramming strategies failed to render iPSCs in vitro and in vivo. Addition of transcriptomic-epigenetic reprogramming “boosters” also failed to generate iPSCs from B cell blasts and B-ALL lines, and when iPSCs emerged they lacked leukemic fusion genes, demonstrating non-leukemic myeloid origin. Conversely, MLL-AF4-overexpressing hematopoietic stem cells/B progenitors were successfully reprogrammed, indicating that B cell origin and leukemic fusion gene were not reprogramming barriers. Global transcriptome/DNA methylome profiling suggested a developmental/differentiation refractoriness of MLL-rearranged B-ALL to reprogramming into pluripotency.

Originele taal-2	Engels
Pagina's (van-tot)	602-618
Aantal pagina's	17
Tijdschrift	Stem Cell Reports
Volume	7
Nummer van het tijdschrift	4
DOI's	https://doi.org/10.1016/j.stemcr.2016.08.013
Status	Gepubliceerd - 11 okt. 2016
Extern gepubliceerd	Ja

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10.1016/j.stemcr.2016.08.013

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Muñoz-López, A., Romero-Moya, D., Prieto, C., Ramos-Mejía, V., Agraz-Doblas, A., Varela, I., Buschbeck, M., Palau, A., Carvajal-Vergara, X., Giorgetti, A., Ford, A., Lako, M., Granada, I., Ruiz-Xivillé, N., Rodríguez-Perales, S., Torres-Ruíz, R., Stam, R. W., Fuster, J. L., Fraga, M. F., ... Menendez, P. (2016). Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency. Stem Cell Reports, 7(4), 602-618. https://doi.org/10.1016/j.stemcr.2016.08.013

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title = "Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency",

abstract = "Induced pluripotent stem cells (iPSCs) are a powerful tool for disease modeling. They are routinely generated from healthy donors and patients from multiple cell types at different developmental stages. However, reprogramming leukemias is an extremely inefficient process. Few studies generated iPSCs from primary chronic myeloid leukemias, but iPSC generation from acute myeloid or lymphoid leukemias (ALL) has not been achieved. We attempted to generate iPSCs from different subtypes of B-ALL to address the developmental impact of leukemic fusion genes. OKSM(L)-expressing mono/polycistronic-, retroviral/lentiviral/episomal-, and Sendai virus vector-based reprogramming strategies failed to render iPSCs in vitro and in vivo. Addition of transcriptomic-epigenetic reprogramming “boosters” also failed to generate iPSCs from B cell blasts and B-ALL lines, and when iPSCs emerged they lacked leukemic fusion genes, demonstrating non-leukemic myeloid origin. Conversely, MLL-AF4-overexpressing hematopoietic stem cells/B progenitors were successfully reprogrammed, indicating that B cell origin and leukemic fusion gene were not reprogramming barriers. Global transcriptome/DNA methylome profiling suggested a developmental/differentiation refractoriness of MLL-rearranged B-ALL to reprogramming into pluripotency.",

keywords = "B-ALL, cancer reprogramming, DNA methylome, iPSC, MLL-AF4, Sendai virus, transcriptome",

author = "Alvaro Mu{\~n}oz-L{\'o}pez and Dami{\`a} Romero-Moya and Cristina Prieto and Ver{\'o}nica Ramos-Mej{\'i}a and Antonio Agraz-Doblas and Ignacio Varela and Marcus Buschbeck and Anna Palau and Xonia Carvajal-Vergara and Alessandra Giorgetti and Anthony Ford and Majlinda Lako and Isabel Granada and Neus Ruiz-Xivill{\'e} and Sandra Rodr{\'i}guez-Perales and Raul Torres-Ru{\'i}z and Stam, {Ronald W.} and Fuster, {Jose Luis} and Fraga, {Mario F.} and Mahito Nakanishi and Gianni Cazzaniga and Michela Bardini and Isabel Cobo and Bayon, {Gustavo F.} and Fernandez, {Agustin F.} and Clara Bueno and Pablo Menendez",

note = "Publisher Copyright: {\textcopyright} 2016 The Authors",

year = "2016",

month = oct,

day = "11",

doi = "10.1016/j.stemcr.2016.08.013",

language = "English",

volume = "7",

pages = "602--618",

journal = "Stem Cell Reports",

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Muñoz-López, A, Romero-Moya, D, Prieto, C, Ramos-Mejía, V, Agraz-Doblas, A, Varela, I, Buschbeck, M, Palau, A, Carvajal-Vergara, X, Giorgetti, A, Ford, A, Lako, M, Granada, I, Ruiz-Xivillé, N, Rodríguez-Perales, S, Torres-Ruíz, R, Stam, RW, Fuster, JL, Fraga, MF, Nakanishi, M, Cazzaniga, G, Bardini, M, Cobo, I, Bayon, GF, Fernandez, AF, Bueno, C & Menendez, P 2016, 'Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency', Stem Cell Reports, vol. 7, nr. 4, blz. 602-618. https://doi.org/10.1016/j.stemcr.2016.08.013

TY - JOUR

T1 - Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency

AU - Muñoz-López, Alvaro

AU - Romero-Moya, Damià

AU - Prieto, Cristina

AU - Ramos-Mejía, Verónica

AU - Agraz-Doblas, Antonio

AU - Varela, Ignacio

AU - Buschbeck, Marcus

AU - Palau, Anna

AU - Carvajal-Vergara, Xonia

AU - Giorgetti, Alessandra

AU - Ford, Anthony

AU - Lako, Majlinda

AU - Granada, Isabel

AU - Ruiz-Xivillé, Neus

AU - Rodríguez-Perales, Sandra

AU - Torres-Ruíz, Raul

AU - Stam, Ronald W.

AU - Fuster, Jose Luis

AU - Fraga, Mario F.

AU - Nakanishi, Mahito

AU - Cazzaniga, Gianni

AU - Bardini, Michela

AU - Cobo, Isabel

AU - Bayon, Gustavo F.

AU - Fernandez, Agustin F.

AU - Bueno, Clara

AU - Menendez, Pablo

PY - 2016/10/11

Y1 - 2016/10/11

N2 - Induced pluripotent stem cells (iPSCs) are a powerful tool for disease modeling. They are routinely generated from healthy donors and patients from multiple cell types at different developmental stages. However, reprogramming leukemias is an extremely inefficient process. Few studies generated iPSCs from primary chronic myeloid leukemias, but iPSC generation from acute myeloid or lymphoid leukemias (ALL) has not been achieved. We attempted to generate iPSCs from different subtypes of B-ALL to address the developmental impact of leukemic fusion genes. OKSM(L)-expressing mono/polycistronic-, retroviral/lentiviral/episomal-, and Sendai virus vector-based reprogramming strategies failed to render iPSCs in vitro and in vivo. Addition of transcriptomic-epigenetic reprogramming “boosters” also failed to generate iPSCs from B cell blasts and B-ALL lines, and when iPSCs emerged they lacked leukemic fusion genes, demonstrating non-leukemic myeloid origin. Conversely, MLL-AF4-overexpressing hematopoietic stem cells/B progenitors were successfully reprogrammed, indicating that B cell origin and leukemic fusion gene were not reprogramming barriers. Global transcriptome/DNA methylome profiling suggested a developmental/differentiation refractoriness of MLL-rearranged B-ALL to reprogramming into pluripotency.

AB - Induced pluripotent stem cells (iPSCs) are a powerful tool for disease modeling. They are routinely generated from healthy donors and patients from multiple cell types at different developmental stages. However, reprogramming leukemias is an extremely inefficient process. Few studies generated iPSCs from primary chronic myeloid leukemias, but iPSC generation from acute myeloid or lymphoid leukemias (ALL) has not been achieved. We attempted to generate iPSCs from different subtypes of B-ALL to address the developmental impact of leukemic fusion genes. OKSM(L)-expressing mono/polycistronic-, retroviral/lentiviral/episomal-, and Sendai virus vector-based reprogramming strategies failed to render iPSCs in vitro and in vivo. Addition of transcriptomic-epigenetic reprogramming “boosters” also failed to generate iPSCs from B cell blasts and B-ALL lines, and when iPSCs emerged they lacked leukemic fusion genes, demonstrating non-leukemic myeloid origin. Conversely, MLL-AF4-overexpressing hematopoietic stem cells/B progenitors were successfully reprogrammed, indicating that B cell origin and leukemic fusion gene were not reprogramming barriers. Global transcriptome/DNA methylome profiling suggested a developmental/differentiation refractoriness of MLL-rearranged B-ALL to reprogramming into pluripotency.

KW - B-ALL

KW - cancer reprogramming

KW - DNA methylome

KW - iPSC

KW - MLL-AF4

KW - Sendai virus

KW - transcriptome

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U2 - 10.1016/j.stemcr.2016.08.013

DO - 10.1016/j.stemcr.2016.08.013

M3 - Article

C2 - 27666791

AN - SCOPUS:84992186929

SN - 2213-6711

VL - 7

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EP - 618

JO - Stem Cell Reports

JF - Stem Cell Reports

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ER -

Development Refractoriness of MLL-Rearranged Human B Cell Acute Leukemias to Reprogramming into Pluripotency

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