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Immunotherapy of Triple-negative Breast Cancer with Cathepsin D-targeting Antibodies

Overview
Journal J Immunother Cancer
Specialties Allergy & Immunology
Oncology
Pharmacology
Date 2019 Feb 6
PMID 30717773
Citations 45
Authors
Yahya Ashraf
Hanane Mansouri
Valerie Laurent-Matha
Lindsay B Alcaraz
Pascal Roger
Severine Guiu
Danielle Derocq
Gautier Robin
Henri-Alexandre Michaud
Helene Delpech
Marta Jarlier
Martine Pugniere
Bruno Robert
Anthony Puel
Lucie Martin
Flavie Landomiel
Thomas Bourquard
Oussama Achour
Ingrid Fruitier-Arnaudin
Alexandre Pichard
Emmanuel Deshayes
Andrei Turtoi
Anne Poupon
Joelle Simony-Lafontaine
Florence Boissiere-Michot
Nelly Pirot
Florence Bernex
William Jacot
Stanislas Du Manoir
Charles Theillet
Jean-Pierre Pouget
Isabelle Navarro-Teulon
Nathalie Bonnefoy
Andre Pelegrin
Thierry Chardes
Pierre Martineau
Emmanuelle Liaudet-Coopman
Affiliations
Soon will be listed here.
Abstract

Background: Triple-negative breast cancer (TNBC) treatment is currently restricted to chemotherapy. Hence, tumor-specific molecular targets and/or alternative therapeutic strategies for TNBC are urgently needed. Immunotherapy is emerging as an exciting treatment option for TNBC patients. The aspartic protease cathepsin D (cath-D), a marker of poor prognosis in breast cancer (BC), is overproduced and hypersecreted by human BC cells. This study explores whether cath-D is a tumor cell-associated extracellular biomarker and a potent target for antibody-based therapy in TNBC.

Methods: Cath-D prognostic value and localization was evaluated by transcriptomics, proteomics and immunohistochemistry in TNBC. First-in-class anti-cath-D human scFv fragments binding to both human and mouse cath-D were generated using phage display and cloned in the human IgG1 λ format (F1 and E2). Anti-cath-D antibody biodistribution, antitumor efficacy and in vivo underlying mechanisms were investigated in TNBC MDA-MB-231 tumor xenografts in nude mice. Antitumor effect was further assessed in TNBC patient-derived xenografts (PDXs).

Results: High CTSD mRNA levels correlated with shorter recurrence-free survival in TNBC, and extracellular cath-D was detected in the tumor microenvironment, but not in matched normal breast stroma. Anti-cath-D F1 and E2 antibodies accumulated in TNBC MDA-MB-231 tumor xenografts, inhibited tumor growth and improved mice survival without apparent toxicity. The Fc function of F1, the best antibody candidate, was essential for maximal tumor inhibition in the MDA-MB-231 model. Mechanistically, F1 antitumor response was triggered through natural killer cell activation via IL-15 upregulation, associated with granzyme B and perforin production, and the release of antitumor IFNγ cytokine. The F1 antibody also prevented the tumor recruitment of immunosuppressive tumor-associated macrophages M2 and myeloid-derived suppressor cells, a specific effect associated with a less immunosuppressive tumor microenvironment highlighted by TGFβ decrease. Finally, the antibody F1 inhibited tumor growth of two TNBC PDXs, isolated from patients resistant or not to neo-adjuvant chemotherapy.

Conclusion: Cath-D is a tumor-specific extracellular target in TNBC suitable for antibody-based therapy. Immunomodulatory antibody-based strategy against cath-D is a promising immunotherapy to treat patients with TNBC.

Citing Articles

Development of a prognostic model based on four genes related to exhausted CD8+ T cell in triple-negative breast cancer patients: a comprehensive analysis integrating scRNA-seq and bulk RNA-seq.

Shi Y, Yu Y, Zhao J, Huang L, Wang Q, Sun Q Discov Oncol. 2025; 16(1):114.

PMID: 39899181 PMC: 11790537. DOI: 10.1007/s12672-025-01812-z.

Antibodies against the multifaceted cathepsin D protein open new avenues for TNBC immunotherapy.

du Roure P, David T, Mallavialle A, Laurent-Matha V, Roger P, Guiu S J Immunother Cancer. 2025; 13(1.

PMID: 39800383 PMC: 11748927. DOI: 10.1136/jitc-2024-009548.

Ubiquitin-specific protease 1 facilitates tumor immune escape from natural killer cells and predicts the prognosis in small cell lung cancer.

Jiang S, Tang Y, Ma F, Niu Y, Sun L Oncol Res. 2024; 33(1):213-224.

PMID: 39735674 PMC: 11671408. DOI: 10.32604/or.2024.046895.

Elucidating Sex-Specific Immune Profiles in a Breast Cancer Model.

Hargrove-Wiley E, Obodo D, Bindeman W, Fingleton B Int J Mol Sci. 2024; 25(23).

PMID: 39684829 PMC: 11641823. DOI: 10.3390/ijms252313113.

Comprehensive pan-cancer analysis reveals ENC1 as a promising prognostic biomarker for tumor microenvironment and therapeutic responses.

Cao Z, Zhu J, Wang Z, Peng Y, Zeng L Sci Rep. 2024; 14(1):25331.

PMID: 39455818 PMC: 11512054. DOI: 10.1038/s41598-024-76798-9.

References
1.
Saadoun H, Lamy P, Thezenas S, Pouderoux S, Bibeau F, Montels F . Prognostic impact of the inclusion of uPA/PAI-1 tumor levels in the current adjuvant treatment decision-making for early breast cancer. Future Oncol. 2014; 10(2):195-209. DOI: 10.2217/fon.13.177. View
2.
Zhao X, Qu J, Sun Y, Wang J, Liu X, Wang F . Prognostic significance of tumor-associated macrophages in breast cancer: a meta-analysis of the literature. Oncotarget. 2017; 8(18):30576-30586. PMC: 5444766. DOI: 10.18632/oncotarget.15736. View
3.
Schmid P, Adams S, Rugo H, Schneeweiss A, Barrios C, Iwata H . Atezolizumab and Nab-Paclitaxel in Advanced Triple-Negative Breast Cancer. N Engl J Med. 2018; 379(22):2108-2121. DOI: 10.1056/NEJMoa1809615. View
4.
Philibert P, Stoessel A, Wang W, Sibler A, Bec N, Larroque C . A focused antibody library for selecting scFvs expressed at high levels in the cytoplasm. BMC Biotechnol. 2007; 7:81. PMC: 2241821. DOI: 10.1186/1472-6750-7-81. View
5.
Ito R, Takahashi T, Katano I, Ito M . Current advances in humanized mouse models. Cell Mol Immunol. 2012; 9(3):208-14. PMC: 4012844. DOI: 10.1038/cmi.2012.2. View