Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms

Siyu Sun; Eunae You; Jungeui Hong; David Hoyos; Isabella Del Priore; Kaloyan M. Tsanov; Om Mattagajasingh; Andrea Di Gioacchino; Sajid A. Marhon; Jonathan Chacon-Barahona; Hao Li; Hua Jiang; Samira Hozeifi; Omar Rosas-Bringas; Katherine H. Xu; Yuhui Song; Evan R. Lang; Alexandra S. Rojas; Linda T. Nieman; Bidish K. Patel; Rajmohan Murali; Pharto Chanda; Ali Karacay; Nicolas Vabret; Daniel D. De Carvalho; Daniel Zenklusen; John LaCava; Scott W. Lowe; David T. Ting; Christine A. Iacobuzio-Donahue; Alexander Solovyov; Benjamin D. Greenbaum

doi:10.1016/j.immuni.2024.10.015

Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms

Siyu Sun^*
, Eunae You
, Jungeui Hong
, David Hoyos
, Isabella Del Priore
, Kaloyan M. Tsanov
, Om Mattagajasingh
, Andrea Di Gioacchino
, Sajid A. Marhon
, Jonathan Chacon-Barahona
, Hao Li
, Hua Jiang
, Samira Hozeifi
, Omar Rosas-Bringas
, Katherine H. Xu
, Yuhui Song
, Evan R. Lang
, Alexandra S. Rojas
, Linda T. Nieman
, Bidish K. Patel

Rajmohan Murali, Pharto Chanda, Ali Karacay, Nicolas Vabret, Daniel D. De Carvalho, Daniel Zenklusen, John LaCava, Scott W. Lowe, David T. Ting, Christine A. Iacobuzio-Donahue, Alexander Solovyov, Benjamin D. Greenbaum^*

^*Corresponding author for this work

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

17 Citations (Scopus)

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Abstract

To thrive, cancer cells must navigate acute inflammatory signaling accompanying oncogenic transformation, such as via overexpression of repeat elements. We examined the relationship between immunostimulatory repeat expression, tumor evolution, and the tumor-immune microenvironment. Integration of multimodal data from a cohort of pancreatic ductal adenocarcinoma (PDAC) patients revealed expression of specific Alu repeats predicted to form double-stranded RNAs (dsRNAs) and trigger retinoic-acid-inducible gene I (RIG-I)-like-receptor (RLR)-associated type-I interferon (IFN) signaling. Such Alu-derived dsRNAs also anti-correlated with pro-tumorigenic macrophage infiltration in late stage tumors. We defined two complementary pathways whereby PDAC may adapt to such anti-tumorigenic signaling. In mutant TP53 tumors, ORF1p from long interspersed nuclear element (LINE)-1 preferentially binds Alus and decreases their expression, whereas adenosine deaminases acting on RNA 1 (ADAR1) editing primarily reduces dsRNA formation in wild-type TP53 tumors. Depletion of either LINE-1 ORF1p or ADAR1 reduced tumor growth in vitro. The fact that tumors utilize multiple pathways to mitigate immunostimulatory repeats implies the stress from their expression is a fundamental phenomenon to which PDAC, and likely other tumors, adapt.

Original language	English
Pages (from-to)	2879-2894.e11
Number of pages	27
Journal	Immunity
Volume	57
Issue number	12
DOIs	https://doi.org/10.1016/j.immuni.2024.10.015
Publication status	Published - 10-Dec-2024

Keywords

ADAR1
cancer evolution
cancer immunity
inverted Alus
retrotransposons
Tp53
tumor-immune microenvironment

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Sun, S., You, E., Hong, J., Hoyos, D., Del Priore, I., Tsanov, K. M., Mattagajasingh, O., Di Gioacchino, A., Marhon, S. A., Chacon-Barahona, J., Li, H., Jiang, H., Hozeifi, S., Rosas-Bringas, O., Xu, K. H., Song, Y., Lang, E. R., Rojas, A. S., Nieman, L. T., ... Greenbaum, B. D. (2024). Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms. Immunity, 57(12), 2879-2894.e11. https://doi.org/10.1016/j.immuni.2024.10.015

@article{c36658dab7744de082e79dadd1d9527f,

title = "Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms",

abstract = "To thrive, cancer cells must navigate acute inflammatory signaling accompanying oncogenic transformation, such as via overexpression of repeat elements. We examined the relationship between immunostimulatory repeat expression, tumor evolution, and the tumor-immune microenvironment. Integration of multimodal data from a cohort of pancreatic ductal adenocarcinoma (PDAC) patients revealed expression of specific Alu repeats predicted to form double-stranded RNAs (dsRNAs) and trigger retinoic-acid-inducible gene I (RIG-I)-like-receptor (RLR)-associated type-I interferon (IFN) signaling. Such Alu-derived dsRNAs also anti-correlated with pro-tumorigenic macrophage infiltration in late stage tumors. We defined two complementary pathways whereby PDAC may adapt to such anti-tumorigenic signaling. In mutant TP53 tumors, ORF1p from long interspersed nuclear element (LINE)-1 preferentially binds Alus and decreases their expression, whereas adenosine deaminases acting on RNA 1 (ADAR1) editing primarily reduces dsRNA formation in wild-type TP53 tumors. Depletion of either LINE-1 ORF1p or ADAR1 reduced tumor growth in vitro. The fact that tumors utilize multiple pathways to mitigate immunostimulatory repeats implies the stress from their expression is a fundamental phenomenon to which PDAC, and likely other tumors, adapt.",

keywords = "ADAR1, cancer evolution, cancer immunity, inverted Alus, retrotransposons, Tp53, tumor-immune microenvironment",

author = "Siyu Sun and Eunae You and Jungeui Hong and David Hoyos and \{Del Priore\}, Isabella and Tsanov, \{Kaloyan M.\} and Om Mattagajasingh and \{Di Gioacchino\}, Andrea and Marhon, \{Sajid A.\} and Jonathan Chacon-Barahona and Hao Li and Hua Jiang and Samira Hozeifi and Omar Rosas-Bringas and Xu, \{Katherine H.\} and Yuhui Song and Lang, \{Evan R.\} and Rojas, \{Alexandra S.\} and Nieman, \{Linda T.\} and Patel, \{Bidish K.\} and Rajmohan Murali and Pharto Chanda and Ali Karacay and Nicolas Vabret and \{De Carvalho\}, \{Daniel D.\} and Daniel Zenklusen and John LaCava and Lowe, \{Scott W.\} and Ting, \{David T.\} and Iacobuzio-Donahue, \{Christine A.\} and Alexander Solovyov and Greenbaum, \{Benjamin D.\}",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors",

year = "2024",

month = dec,

day = "10",

doi = "10.1016/j.immuni.2024.10.015",

language = "English",

volume = "57",

pages = "2879--2894.e11",

journal = "Immunity",

issn = "1074-7613",

publisher = "Cell Press",

number = "12",

}

Sun, S, You, E, Hong, J, Hoyos, D, Del Priore, I, Tsanov, KM, Mattagajasingh, O, Di Gioacchino, A, Marhon, SA, Chacon-Barahona, J, Li, H, Jiang, H, Hozeifi, S, Rosas-Bringas, O, Xu, KH, Song, Y, Lang, ER, Rojas, AS, Nieman, LT, Patel, BK, Murali, R, Chanda, P, Karacay, A, Vabret, N, De Carvalho, DD, Zenklusen, D, LaCava, J, Lowe, SW, Ting, DT, Iacobuzio-Donahue, CA, Solovyov, A & Greenbaum, BD 2024, 'Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms', Immunity, vol. 57, no. 12, pp. 2879-2894.e11. https://doi.org/10.1016/j.immuni.2024.10.015

TY - JOUR

T1 - Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms

AU - Sun, Siyu

AU - You, Eunae

AU - Hong, Jungeui

AU - Hoyos, David

AU - Del Priore, Isabella

AU - Tsanov, Kaloyan M.

AU - Mattagajasingh, Om

AU - Di Gioacchino, Andrea

AU - Marhon, Sajid A.

AU - Chacon-Barahona, Jonathan

AU - Li, Hao

AU - Jiang, Hua

AU - Hozeifi, Samira

AU - Rosas-Bringas, Omar

AU - Xu, Katherine H.

AU - Song, Yuhui

AU - Lang, Evan R.

AU - Rojas, Alexandra S.

AU - Nieman, Linda T.

AU - Patel, Bidish K.

AU - Murali, Rajmohan

AU - Chanda, Pharto

AU - Karacay, Ali

AU - Vabret, Nicolas

AU - De Carvalho, Daniel D.

AU - Zenklusen, Daniel

AU - LaCava, John

AU - Lowe, Scott W.

AU - Ting, David T.

AU - Iacobuzio-Donahue, Christine A.

AU - Solovyov, Alexander

AU - Greenbaum, Benjamin D.

PY - 2024/12/10

Y1 - 2024/12/10

N2 - To thrive, cancer cells must navigate acute inflammatory signaling accompanying oncogenic transformation, such as via overexpression of repeat elements. We examined the relationship between immunostimulatory repeat expression, tumor evolution, and the tumor-immune microenvironment. Integration of multimodal data from a cohort of pancreatic ductal adenocarcinoma (PDAC) patients revealed expression of specific Alu repeats predicted to form double-stranded RNAs (dsRNAs) and trigger retinoic-acid-inducible gene I (RIG-I)-like-receptor (RLR)-associated type-I interferon (IFN) signaling. Such Alu-derived dsRNAs also anti-correlated with pro-tumorigenic macrophage infiltration in late stage tumors. We defined two complementary pathways whereby PDAC may adapt to such anti-tumorigenic signaling. In mutant TP53 tumors, ORF1p from long interspersed nuclear element (LINE)-1 preferentially binds Alus and decreases their expression, whereas adenosine deaminases acting on RNA 1 (ADAR1) editing primarily reduces dsRNA formation in wild-type TP53 tumors. Depletion of either LINE-1 ORF1p or ADAR1 reduced tumor growth in vitro. The fact that tumors utilize multiple pathways to mitigate immunostimulatory repeats implies the stress from their expression is a fundamental phenomenon to which PDAC, and likely other tumors, adapt.

AB - To thrive, cancer cells must navigate acute inflammatory signaling accompanying oncogenic transformation, such as via overexpression of repeat elements. We examined the relationship between immunostimulatory repeat expression, tumor evolution, and the tumor-immune microenvironment. Integration of multimodal data from a cohort of pancreatic ductal adenocarcinoma (PDAC) patients revealed expression of specific Alu repeats predicted to form double-stranded RNAs (dsRNAs) and trigger retinoic-acid-inducible gene I (RIG-I)-like-receptor (RLR)-associated type-I interferon (IFN) signaling. Such Alu-derived dsRNAs also anti-correlated with pro-tumorigenic macrophage infiltration in late stage tumors. We defined two complementary pathways whereby PDAC may adapt to such anti-tumorigenic signaling. In mutant TP53 tumors, ORF1p from long interspersed nuclear element (LINE)-1 preferentially binds Alus and decreases their expression, whereas adenosine deaminases acting on RNA 1 (ADAR1) editing primarily reduces dsRNA formation in wild-type TP53 tumors. Depletion of either LINE-1 ORF1p or ADAR1 reduced tumor growth in vitro. The fact that tumors utilize multiple pathways to mitigate immunostimulatory repeats implies the stress from their expression is a fundamental phenomenon to which PDAC, and likely other tumors, adapt.

KW - ADAR1

KW - cancer evolution

KW - cancer immunity

KW - inverted Alus

KW - retrotransposons

KW - Tp53

KW - tumor-immune microenvironment

UR - https://www.scopus.com/pages/publications/85211038227

U2 - 10.1016/j.immuni.2024.10.015

DO - 10.1016/j.immuni.2024.10.015

M3 - Article

C2 - 39577413

AN - SCOPUS:85211038227

SN - 1074-7613

VL - 57

SP - 2879-2894.e11

JO - Immunity

JF - Immunity

IS - 12

ER -

Cancer cells restrict immunogenicity of retrotransposon expression via distinct mechanisms

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