Tumor-Infiltrating Clonal Hematopoiesis

Oriol Pich; Elsa Bernard; Maria Zagorulya; Andrew Rowan; Constandina Pospori; Ramy Slama; Hector Huerga Encabo; Jennifer O'Sullivan; Despoina Papazoglou; Panayiotis Anastasiou; Chrysante S. Iliakis; Sally Ann Clark; Krijn K. Dijkstra; Vittorio Barbè; Chris Bailey; Aaron J. Stonestrom; Katey S.S. Enfield; Mary Green; Charlotte K. Brierley; Alastair Magness; David R. Pearce; Robert E. Hynds; Rija Zaidi; Jayant K. Rane; Ángel F. Álvarez-Prado; Kerstin Thol; Rachel Scott; Supreet Kaur Bola; Elena Hoxha; Steve K. Harris; Karl S. Peggs; Sergio A. Quezada; Allan Hackshaw; Simone Zaccaria; Johanna A. Joyce; Ilaria Malanchi; Michael F. Berger; Mariam Jamal-Hanjani; Andreas Wack; Julian Downward; William Grey; Cristina Lo Celso; Eva Grönroos; Charles M. Rudin; Adam J. Mead; Dominique Bonnet; Elli Papaemmanuil; Charles Swanton

doi:10.1056/NEJMoa2413361

Tumor-Infiltrating Clonal Hematopoiesis

Oriol Pich, Elsa Bernard, Maria Zagorulya, Andrew Rowan, Constandina Pospori, Ramy Slama, Hector Huerga Encabo, Jennifer O'Sullivan, Despoina Papazoglou, Panayiotis Anastasiou, Chrysante S. Iliakis, Sally Ann Clark, Krijn K. Dijkstra, Vittorio Barbè, Chris Bailey, Aaron J. Stonestrom, Katey S.S. Enfield, Mary Green, Charlotte K. Brierley, Alastair MagnessDavid R. Pearce, Robert E. Hynds, Rija Zaidi, Jayant K. Rane, Ángel F. Álvarez-Prado, Kerstin Thol, Rachel Scott, Supreet Kaur Bola, Elena Hoxha, Steve K. Harris, Karl S. Peggs, Sergio A. Quezada, Allan Hackshaw, Simone Zaccaria, Johanna A. Joyce, Ilaria Malanchi, Michael F. Berger, Mariam Jamal-Hanjani, Andreas Wack, Julian Downward, William Grey, Cristina Lo Celso, Eva Grönroos, Charles M. Rudin, Adam J. Mead, Dominique Bonnet, Elli Papaemmanuil, Charles Swanton

Résultats de recherche: Contribution à un journal › Article › Revue par des pairs

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Résumé

BACKGROUND: Clonal hematopoiesis of indeterminate potential (CHIP) is an age-related condition associated with increased mortality among patients with cancer. CHIP mutations with high variant-allele frequencies can be detected in tumors, a phenomenon we term tumor-infiltrating clonal hematopoiesis (TI-CH). The frequency of TI-CH and its effect on tumor evolution are unclear. METHODS: We characterized CHIP and TI-CH in 421 patients with early-stage non-small-cell lung cancer (NSCLC) from the TRACERx study and in 49,351 patients from the MSK-IMPACT pan-cancer cohort. We studied the association of TI-CH with survival and disease recurrence and evaluated the functional effect of TET2-mutant CHIP on the biologic features of lung tumors. RESULTS: Among patients with NSCLC, 42% of those with CHIP had TI-CH. TI-CH independently predicted an increased risk of death or recurrence, with an adjusted hazard ratio of 1.80 (95% confidence interval [CI], 1.23 to 2.63) as compared with the absence of CHIP and an adjusted hazard ratio of 1.62 (95% CI, 1.02 to 2.56) as compared with CHIP in the absence of TI-CH. Among patients with solid tumors, 26% of those with CHIP had TI-CH. TI-CH conferred a risk of death from any cause that was 1.17 times (95% CI, 1.06 to 1.29) as high as the risk with CHIP in the absence of TI-CH. TET2 mutations were the strongest genetic predictor of TI-CH; such mutations enhanced monocyte migration to lung tumor cells, fueled a myeloid-rich tumor microenvironment in mice, and resulted in the promotion of tumor organoid growth. CONCLUSIONS: TI-CH increased the risk of disease recurrence or death among patients with NSCLC and the risk of death from any cause among patients with solid tumors. TI-CH remodeled the tumor immune microenvironment and accelerated tumor organoid growth, findings that support a role for an aging-related hematologic clonal proliferation in cancer evolution. (Funded by the Royal Society and others.).

langue originale	Anglais
Pages (de - à)	1594-1608
Nombre de pages	15
journal	New England Journal of Medicine
Volume	392
Numéro de publication	16
Les DOIs	https://doi.org/10.1056/NEJMoa2413361
état	Publié - 24 avr. 2025

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10.1056/NEJMoa2413361

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Pich, O., Bernard, E., Zagorulya, M., Rowan, A., Pospori, C., Slama, R., Huerga Encabo, H., O'Sullivan, J., Papazoglou, D., Anastasiou, P., Iliakis, C. S., Clark, S. A., Dijkstra, K. K., Barbè, V., Bailey, C., Stonestrom, A. J., Enfield, K. S. S., Green, M., Brierley, C. K., ... Swanton, C. (2025). Tumor-Infiltrating Clonal Hematopoiesis. New England Journal of Medicine, 392(16), 1594-1608. https://doi.org/10.1056/NEJMoa2413361

@article{f127822e2a9e4a8784e91e28bf4eec2e,

title = "Tumor-Infiltrating Clonal Hematopoiesis",

abstract = "BACKGROUND: Clonal hematopoiesis of indeterminate potential (CHIP) is an age-related condition associated with increased mortality among patients with cancer. CHIP mutations with high variant-allele frequencies can be detected in tumors, a phenomenon we term tumor-infiltrating clonal hematopoiesis (TI-CH). The frequency of TI-CH and its effect on tumor evolution are unclear. METHODS: We characterized CHIP and TI-CH in 421 patients with early-stage non-small-cell lung cancer (NSCLC) from the TRACERx study and in 49,351 patients from the MSK-IMPACT pan-cancer cohort. We studied the association of TI-CH with survival and disease recurrence and evaluated the functional effect of TET2-mutant CHIP on the biologic features of lung tumors. RESULTS: Among patients with NSCLC, 42% of those with CHIP had TI-CH. TI-CH independently predicted an increased risk of death or recurrence, with an adjusted hazard ratio of 1.80 (95% confidence interval [CI], 1.23 to 2.63) as compared with the absence of CHIP and an adjusted hazard ratio of 1.62 (95% CI, 1.02 to 2.56) as compared with CHIP in the absence of TI-CH. Among patients with solid tumors, 26% of those with CHIP had TI-CH. TI-CH conferred a risk of death from any cause that was 1.17 times (95% CI, 1.06 to 1.29) as high as the risk with CHIP in the absence of TI-CH. TET2 mutations were the strongest genetic predictor of TI-CH; such mutations enhanced monocyte migration to lung tumor cells, fueled a myeloid-rich tumor microenvironment in mice, and resulted in the promotion of tumor organoid growth. CONCLUSIONS: TI-CH increased the risk of disease recurrence or death among patients with NSCLC and the risk of death from any cause among patients with solid tumors. TI-CH remodeled the tumor immune microenvironment and accelerated tumor organoid growth, findings that support a role for an aging-related hematologic clonal proliferation in cancer evolution. (Funded by the Royal Society and others.).",

author = "Oriol Pich and Elsa Bernard and Maria Zagorulya and Andrew Rowan and Constandina Pospori and Ramy Slama and {Huerga Encabo}, Hector and Jennifer O'Sullivan and Despoina Papazoglou and Panayiotis Anastasiou and Iliakis, {Chrysante S.} and Clark, {Sally Ann} and Dijkstra, {Krijn K.} and Vittorio Barb{\`e} and Chris Bailey and Stonestrom, {Aaron J.} and Enfield, {Katey S.S.} and Mary Green and Brierley, {Charlotte K.} and Alastair Magness and Pearce, {David R.} and Hynds, {Robert E.} and Rija Zaidi and Rane, {Jayant K.} and {\'A}lvarez-Prado, {{\'A}ngel F.} and Kerstin Thol and Rachel Scott and Bola, {Supreet Kaur} and Elena Hoxha and Harris, {Steve K.} and Peggs, {Karl S.} and Quezada, {Sergio A.} and Allan Hackshaw and Simone Zaccaria and Joyce, {Johanna A.} and Ilaria Malanchi and Berger, {Michael F.} and Mariam Jamal-Hanjani and Andreas Wack and Julian Downward and William Grey and {Lo Celso}, Cristina and Eva Gr{\"o}nroos and Rudin, {Charles M.} and Mead, {Adam J.} and Dominique Bonnet and Elli Papaemmanuil and Charles Swanton",

note = "Publisher Copyright: Copyright {\textcopyright} 2025 Massachusetts Medical Society.",

year = "2025",

month = apr,

day = "24",

doi = "10.1056/NEJMoa2413361",

language = "English",

volume = "392",

pages = "1594--1608",

journal = "New England Journal of Medicine",

issn = "0028-4793",

number = "16",

}

Pich, O, Bernard, E, Zagorulya, M, Rowan, A, Pospori, C, Slama, R, Huerga Encabo, H, O'Sullivan, J, Papazoglou, D, Anastasiou, P, Iliakis, CS, Clark, SA, Dijkstra, KK, Barbè, V, Bailey, C, Stonestrom, AJ, Enfield, KSS, Green, M, Brierley, CK, Magness, A, Pearce, DR, Hynds, RE, Zaidi, R, Rane, JK, Álvarez-Prado, ÁF, Thol, K, Scott, R, Bola, SK, Hoxha, E, Harris, SK, Peggs, KS, Quezada, SA, Hackshaw, A, Zaccaria, S, Joyce, JA, Malanchi, I, Berger, MF, Jamal-Hanjani, M, Wack, A, Downward, J, Grey, W, Lo Celso, C, Grönroos, E, Rudin, CM, Mead, AJ, Bonnet, D, Papaemmanuil, E & Swanton, C 2025, 'Tumor-Infiltrating Clonal Hematopoiesis', New England Journal of Medicine, VOL. 392, Numéro 16, p. 1594-1608. https://doi.org/10.1056/NEJMoa2413361

TY - JOUR

T1 - Tumor-Infiltrating Clonal Hematopoiesis

AU - Pich, Oriol

AU - Bernard, Elsa

AU - Zagorulya, Maria

AU - Rowan, Andrew

AU - Pospori, Constandina

AU - Slama, Ramy

AU - Huerga Encabo, Hector

AU - O'Sullivan, Jennifer

AU - Papazoglou, Despoina

AU - Anastasiou, Panayiotis

AU - Iliakis, Chrysante S.

AU - Clark, Sally Ann

AU - Dijkstra, Krijn K.

AU - Barbè, Vittorio

AU - Bailey, Chris

AU - Stonestrom, Aaron J.

AU - Enfield, Katey S.S.

AU - Green, Mary

AU - Brierley, Charlotte K.

AU - Magness, Alastair

AU - Pearce, David R.

AU - Hynds, Robert E.

AU - Zaidi, Rija

AU - Rane, Jayant K.

AU - Álvarez-Prado, Ángel F.

AU - Thol, Kerstin

AU - Scott, Rachel

AU - Bola, Supreet Kaur

AU - Hoxha, Elena

AU - Harris, Steve K.

AU - Peggs, Karl S.

AU - Quezada, Sergio A.

AU - Hackshaw, Allan

AU - Zaccaria, Simone

AU - Joyce, Johanna A.

AU - Malanchi, Ilaria

AU - Berger, Michael F.

AU - Jamal-Hanjani, Mariam

AU - Wack, Andreas

AU - Downward, Julian

AU - Grey, William

AU - Lo Celso, Cristina

AU - Grönroos, Eva

AU - Rudin, Charles M.

AU - Mead, Adam J.

AU - Bonnet, Dominique

AU - Papaemmanuil, Elli

AU - Swanton, Charles

PY - 2025/4/24

Y1 - 2025/4/24

N2 - BACKGROUND: Clonal hematopoiesis of indeterminate potential (CHIP) is an age-related condition associated with increased mortality among patients with cancer. CHIP mutations with high variant-allele frequencies can be detected in tumors, a phenomenon we term tumor-infiltrating clonal hematopoiesis (TI-CH). The frequency of TI-CH and its effect on tumor evolution are unclear. METHODS: We characterized CHIP and TI-CH in 421 patients with early-stage non-small-cell lung cancer (NSCLC) from the TRACERx study and in 49,351 patients from the MSK-IMPACT pan-cancer cohort. We studied the association of TI-CH with survival and disease recurrence and evaluated the functional effect of TET2-mutant CHIP on the biologic features of lung tumors. RESULTS: Among patients with NSCLC, 42% of those with CHIP had TI-CH. TI-CH independently predicted an increased risk of death or recurrence, with an adjusted hazard ratio of 1.80 (95% confidence interval [CI], 1.23 to 2.63) as compared with the absence of CHIP and an adjusted hazard ratio of 1.62 (95% CI, 1.02 to 2.56) as compared with CHIP in the absence of TI-CH. Among patients with solid tumors, 26% of those with CHIP had TI-CH. TI-CH conferred a risk of death from any cause that was 1.17 times (95% CI, 1.06 to 1.29) as high as the risk with CHIP in the absence of TI-CH. TET2 mutations were the strongest genetic predictor of TI-CH; such mutations enhanced monocyte migration to lung tumor cells, fueled a myeloid-rich tumor microenvironment in mice, and resulted in the promotion of tumor organoid growth. CONCLUSIONS: TI-CH increased the risk of disease recurrence or death among patients with NSCLC and the risk of death from any cause among patients with solid tumors. TI-CH remodeled the tumor immune microenvironment and accelerated tumor organoid growth, findings that support a role for an aging-related hematologic clonal proliferation in cancer evolution. (Funded by the Royal Society and others.).

AB - BACKGROUND: Clonal hematopoiesis of indeterminate potential (CHIP) is an age-related condition associated with increased mortality among patients with cancer. CHIP mutations with high variant-allele frequencies can be detected in tumors, a phenomenon we term tumor-infiltrating clonal hematopoiesis (TI-CH). The frequency of TI-CH and its effect on tumor evolution are unclear. METHODS: We characterized CHIP and TI-CH in 421 patients with early-stage non-small-cell lung cancer (NSCLC) from the TRACERx study and in 49,351 patients from the MSK-IMPACT pan-cancer cohort. We studied the association of TI-CH with survival and disease recurrence and evaluated the functional effect of TET2-mutant CHIP on the biologic features of lung tumors. RESULTS: Among patients with NSCLC, 42% of those with CHIP had TI-CH. TI-CH independently predicted an increased risk of death or recurrence, with an adjusted hazard ratio of 1.80 (95% confidence interval [CI], 1.23 to 2.63) as compared with the absence of CHIP and an adjusted hazard ratio of 1.62 (95% CI, 1.02 to 2.56) as compared with CHIP in the absence of TI-CH. Among patients with solid tumors, 26% of those with CHIP had TI-CH. TI-CH conferred a risk of death from any cause that was 1.17 times (95% CI, 1.06 to 1.29) as high as the risk with CHIP in the absence of TI-CH. TET2 mutations were the strongest genetic predictor of TI-CH; such mutations enhanced monocyte migration to lung tumor cells, fueled a myeloid-rich tumor microenvironment in mice, and resulted in the promotion of tumor organoid growth. CONCLUSIONS: TI-CH increased the risk of disease recurrence or death among patients with NSCLC and the risk of death from any cause among patients with solid tumors. TI-CH remodeled the tumor immune microenvironment and accelerated tumor organoid growth, findings that support a role for an aging-related hematologic clonal proliferation in cancer evolution. (Funded by the Royal Society and others.).

UR - http://www.scopus.com/inward/record.url?scp=105003982175&partnerID=8YFLogxK

U2 - 10.1056/NEJMoa2413361

DO - 10.1056/NEJMoa2413361

M3 - Article

C2 - 40267425

AN - SCOPUS:105003982175

SN - 0028-4793

VL - 392

SP - 1594

EP - 1608

JO - New England Journal of Medicine

JF - New England Journal of Medicine

IS - 16

ER -