Nanofitins targeting heat shock protein 110: an innovative immunotherapeutic modality in cancer.

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RESEARCH PRODUCT

Nanofitins targeting heat shock protein 110: an innovative immunotherapeutic modality in cancer.

Mathieu Moreau Olivier Kitten Alexandre M.m. Dias Alexandre M.m. Dias Renaud Seigneuric Renaud Seigneuric Jessica Gobbo Jessica Gobbo François Hermetet François Hermetet Fabrice Neiers Fabrice Neiers Pierre-simon Bellaye Bertrand Collin Lucile Dondaine Lucile Dondaine Guillaume Marcion Guillaume Marcion Mathieu Cinier Loïc Briand Loïc Briand Laurène Da Costa Burhan Uyanik Burhan Uyanik Carmen Garrido Carmen Garrido

subject

Cancer Research Mice 03 medical and health sciences Lymphocytes Tumor-Infiltrating 0302 clinical medicine Immune system Peptide Library In vivo Cell Line Tumor Heat shock protein Tumor Microenvironment medicine Animals Humans Cytotoxic T cell HSP110 Heat-Shock Proteins small peptide molecules Tumor microenvironment anticancer targeted therapy biology Chemistry Macrophages Cancer [SDV.SP]Life Sciences [q-bio]/Pharmaceutical sciences medicine.disease Xenograft Model Antitumor Assays Peptide Fragments In vitro 3. Good health Nanofitins Oncology Positron-Emission Tomography 030220 oncology & carcinogenesis biology.protein Cancer research Female Antibody Colorectal Neoplasms HSP110

description

The presence of an inactivating heat shock protein 110 (HSP110) mutation in colorectal cancers has been correlated with an excellent prognosis and with the ability of HSP110 to favor the formation of tolerogenic (M2-like) macrophages. These clinical and experimental results suggest a potentially powerful new strategy against colorectal cancer: the inhibition of HSP110. In this work, as an alternative to neutralizing antibodies, Nanofitins (scaffold ~7 kDa proteins) targeting HSP110 were isolated from the screening of a synthetic Nanofitin library, and their capacity to bind (immunoprecipitation, biolayer interferometry) and to inhibit HSP110 was analyzed in vitro and in vivo. Three Nanofitins were found to inhibit HSP110 chaperone activity. Interestingly, they share a high degree of homology in their variable domain and target the peptide-binding domain of HSP110. In vitro, they inhibited the ability of HSP110 to favor M2-like macrophages. The Nanofitin with the highest affinity, A-C2, was studied in the CT26 colorectal cancer mice model. Our PET/scan experiments demonstrate that A-C2 may be localized within the tumor area, in accordance with the reported HSP110 abundance in the tumor microenvironment. A-C2 treatment reduced tumor growth and was associated with an increase in immune cells infiltrating the tumor and particularly cytotoxic macrophages. These results were confirmed in a chicken chorioallantoic membrane tumor model. Finally, we showed the complementarity between A-C2 and an anti-PD-L1 strategy in the in vivo and in ovo tumor models. Overall, Nanofitins appear to be promising new immunotherapeutic lead compounds.

year	journal	country	edition	language
2021-06-01

10.1002/ijc.33485 https://hal.inrae.fr/hal-03144438