A constitutive interferon-high immunophenotype defines response to immunotherapy in colorectal cancer

Acha-Sagredo, A.; Andrei, P.; Clayton, K.; Taggart, E.; Antoniotti, C.; Woodman, C.A.; Afrache, H.; Fourny, C.; Armero, M.; Moinudeen, H.K.; Green, M.; Bhardwaj, N.; Mikolajczak, A.; Rodriguez-Lopez, M.; Crawford, M.; Connick, E.; Lim, S.; Hobson, P.; Linares, J.; Ignatova, E.; Pelka, D.; Smyth, E.C.; Diamantis, N.; Sosnowska, D.; Carullo, M.; Ciraci, P.; Bergamo, F.; Intini, R.; Nye, E.; Barral, P.; Mishto, M.; Arnold, J.N.; Lonardi, S.; Cremolini, C.; Fontana, E.; Rodriguez-Justo, M.; Ciccarelli, F.D.

doi:10.1016/j.ccell.2024.12.008

Fewer than 50% of metastatic deficient mismatch repair (dMMR) colorectal cancer (CRC) patients respond to immune checkpoint inhibition (ICI). Identifying and expanding this patient population remains a pressing clinical need. Here, we report that an interferon-high immunophenotype locally enriched in cytotoxic lymphocytes and antigen-presenting macrophages is required for response. This immunophenotype is not exclusive to dMMR CRCs but comprises a subset of MMR proficient (pMMR) CRCs. Single-cell spatial analysis and in vitro cell co-cultures indicate that interferon-producing cytotoxic T cells induce overexpression of antigen presentation in adjacent macrophages and tumor cells, including MHC class II invariant chain CD74. dMMR CRCs expressing high levels of CD74 respond to ICI and a subset of CD74 high pMMR CRC patients show better progression free survival when treated with ICI. Therefore, CD74 abundance can identify the constitutive interferon-high immunophenotype determining clinical benefit in CRC, independently of tumor mutational burden or MMR status.

A constitutive interferon-high immunophenotype defines response to immunotherapy in colorectal cancer / A. Acha-Sagredo, P. Andrei, K. Clayton, E. Taggart, C. Antoniotti, C.A. Woodman, H. Afrache, C. Fourny, M. Armero, H.K. Moinudeen, M. Green, N. Bhardwaj, A. Mikolajczak, M. Rodriguez-Lopez, M. Crawford, E. Connick, S. Lim, P. Hobson, J. Linares, E. Ignatova, D. Pelka, E.C. Smyth, N. Diamantis, D. Sosnowska, M. Carullo, P. Ciraci, F. Bergamo, R. Intini, E. Nye, P. Barral, M. Mishto, J.N. Arnold, S. Lonardi, C. Cremolini, E. Fontana, M. Rodriguez-Justo, F.D. Ciccarelli. - In: CANCER CELL. - ISSN 1535-6108. - 43:2(2025 Feb 10), pp. 292-307.e7. [10.1016/j.ccell.2024.12.008]

A constitutive interferon-high immunophenotype defines response to immunotherapy in colorectal cancer

Acha-Sagredo A.^Primo;Andrei P.^Secondo;Clayton K.;Taggart E.;Antoniotti C.;Woodman C. A.;Afrache H.;Fourny C.;Armero M.;Moinudeen H. K.;Green M.;Bhardwaj N.;Mikolajczak A.;Rodriguez-Lopez M.;Crawford M.;Connick E.;Lim S.;Hobson P.;Linares J.;Ignatova E.;Pelka D.;Smyth E. C.;Diamantis N.;Sosnowska D.;Carullo M.;Ciraci P.;Bergamo F.;Intini R.;Nye E.;Barral P.;Mishto M.;Arnold J. N.;Lonardi S.;Cremolini C.;Fontana E.;Rodriguez-Justo M.^Penultimo;F.D. Ciccarelli^{Ultimo

Conceptualization}

2025

Abstract

Fewer than 50% of metastatic deficient mismatch repair (dMMR) colorectal cancer (CRC) patients respond to immune checkpoint inhibition (ICI). Identifying and expanding this patient population remains a pressing clinical need. Here, we report that an interferon-high immunophenotype locally enriched in cytotoxic lymphocytes and antigen-presenting macrophages is required for response. This immunophenotype is not exclusive to dMMR CRCs but comprises a subset of MMR proficient (pMMR) CRCs. Single-cell spatial analysis and in vitro cell co-cultures indicate that interferon-producing cytotoxic T cells induce overexpression of antigen presentation in adjacent macrophages and tumor cells, including MHC class II invariant chain CD74. dMMR CRCs expressing high levels of CD74 respond to ICI and a subset of CD74 high pMMR CRC patients show better progression free survival when treated with ICI. Therefore, CD74 abundance can identify the constitutive interferon-high immunophenotype determining clinical benefit in CRC, independently of tumor mutational burden or MMR status.

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	Parole chiave
	
				antigen presentation; CD74; colorectal cancer; immunotherapy; interferon; marker of response; patient stratification; spatial transcriptomics; tumor immune microenvironment;
			
	Settori scientifico-disciplinari dell'articolo (validi dal 09/05/2024)
	
				Settore BIOS-08/A - Biologia molecolare
			
	Titolo del progetto
	
	Titolo Progetto
	
									Three-dimensional matrices and engineered nanoparticles for locoregional treatment of hepatocellular carcinoma (ManoHCC)
								
	Acronimo
	
									ManoHCC
								
	Nome finanziatore
	
										UNIVERSITA' DEGLI STUDI DI MODENA E REGGIO EMILIA
									
	N. Contratto
	
									PE00000019
								
	Data di pubblicazione
	
				10-feb-2025
			
	Rivista in ANCE
	
				CANCER CELL
			
	DOI
	
				https://dx.doi.org/10.1016/j.ccell.2024.12.008
			
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				01 - Articolo su periodico

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