Anti-MIF nanobodies as a novel tool to improve cancer therapy

Romina Mora Barthelmess; Benoit Stijlemans; Jo Van Ginderachter

Anti-MIF nanobodies as a novel tool to improve cancer therapy

Romina Mora Barthelmess, Benoit Stijlemans, Jo Van Ginderachter

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The macrophage migration inhibitory factor or MIF is a multifunctional cytokine that once bound to CD74, its main receptor, promotes the expression of pro-inflammatory cytokines, angiogenesis, and cell survival among other functions. MIF has been implicated as a biomarker of different diseases that have an inflammatory component, such as autoimmune diseases, metabolic disorders, systemic infections, and cancer. In this context, cross-reactive anti-MIF nanobodies (Nbs) were developed, and 11 different Nbs belonging to 7 different families were selected. We found that 2 out of the 11 Nbs significantly reduced TNF expression of murine and human LPS-stimulated cells. Interestingly, by generating tri-valent constructs, having anti-MIF Nbs on the ends and an anti-albumin Nb in the middle, to increase the half-life, the TNF expression was further reduced. More importantly, the tri-valent constructs were shown to be protective in a murine endotoxemia model, increasing mice survival. Based on these results and taking into consideration MIF’s pro-tumoral role, we decided to test whether these constructs can reduce tumor growth as monotherapy or increase the efficacy of current immunotherapies, such as PD-1 antibodies. We found that the anti-MIF monotherapy significantly reduces tumor growth compared to the untreated and the anti-PD-1 treated groups. The group receiving anti-MIF + anti-PD-1 also showed a slower growth compared to the untreated group, and the anti-PD-1 group, however, there are no significant differences between the mono- and combinatorial treatment regarding tumor growth, suggesting no additional contribution of the anti-PD-1 treatment. Within the tumor microenvironment, we found a significant increase of CD45+cells, CD4+ T cells, and IFN-γ CD8+ producing cells in the anti-MIF + anti-PD-1 treated group compared to the other groups. As a next step, we will include models which are less responsive to immunotherapy, where new alternatives are highly needed.

Originele taal-2	English
Status	Unpublished - 19 sep 2022
Evenement	35th Conference of the European Macrophage and Dendritic cell Society - University of Bonn, Bonn, Germany Duur: 19 sep 2022 → 21 sep 2022 Congresnummer: 35th https://www.emds2022.com/

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Conference	35th Conference of the European Macrophage and Dendritic cell Society
Verkorte titel	EMDS
Land/Regio	Germany
Stad	Bonn
Periode	19/09/22 → 21/09/22
Internet adres	https://www.emds2022.com/

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@conference{d181d5664fe040faa050ae12d0d739b5,

title = "Anti-MIF nanobodies as a novel tool to improve cancer therapy",

abstract = "The macrophage migration inhibitory factor or MIF is a multifunctional cytokine that once bound to CD74, its main receptor, promotes the expression of pro-inflammatory cytokines, angiogenesis, and cell survival among other functions. MIF has been implicated as a biomarker of different diseases that have an inflammatory component, such as autoimmune diseases, metabolic disorders, systemic infections, and cancer. In this context, cross-reactive anti-MIF nanobodies (Nbs) were developed, and 11 different Nbs belonging to 7 different families were selected. We found that 2 out of the 11 Nbs significantly reduced TNF expression of murine and human LPS-stimulated cells. Interestingly, by generating tri-valent constructs, having anti-MIF Nbs on the ends and an anti-albumin Nb in the middle, to increase the half-life, the TNF expression was further reduced. More importantly, the tri-valent constructs were shown to be protective in a murine endotoxemia model, increasing mice survival. Based on these results and taking into consideration MIF{\textquoteright}s pro-tumoral role, we decided to test whether these constructs can reduce tumor growth as monotherapy or increase the efficacy of current immunotherapies, such as PD-1 antibodies. We found that the anti-MIF monotherapy significantly reduces tumor growth compared to the untreated and the anti-PD-1 treated groups. The group receiving anti-MIF + anti-PD-1 also showed a slower growth compared to the untreated group, and the anti-PD-1 group, however, there are no significant differences between the mono- and combinatorial treatment regarding tumor growth, suggesting no additional contribution of the anti-PD-1 treatment. Within the tumor microenvironment, we found a significant increase of CD45+cells, CD4+ T cells, and IFN-γ CD8+ producing cells in the anti-MIF + anti-PD-1 treated group compared to the other groups. As a next step, we will include models which are less responsive to immunotherapy, where new alternatives are highly needed.",

author = "{Mora Barthelmess}, Romina and Benoit Stijlemans and {Van Ginderachter}, Jo",

year = "2022",

month = sep,

day = "19",

language = "English",

note = "35th Conference of the European Macrophage and Dendritic cell Society, EMDS ; Conference date: 19-09-2022 Through 21-09-2022",

url = "https://www.emds2022.com/",

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TY - CONF

T1 - Anti-MIF nanobodies as a novel tool to improve cancer therapy

AU - Mora Barthelmess, Romina

AU - Stijlemans, Benoit

AU - Van Ginderachter, Jo

N1 - Conference code: 35th

PY - 2022/9/19

Y1 - 2022/9/19

N2 - The macrophage migration inhibitory factor or MIF is a multifunctional cytokine that once bound to CD74, its main receptor, promotes the expression of pro-inflammatory cytokines, angiogenesis, and cell survival among other functions. MIF has been implicated as a biomarker of different diseases that have an inflammatory component, such as autoimmune diseases, metabolic disorders, systemic infections, and cancer. In this context, cross-reactive anti-MIF nanobodies (Nbs) were developed, and 11 different Nbs belonging to 7 different families were selected. We found that 2 out of the 11 Nbs significantly reduced TNF expression of murine and human LPS-stimulated cells. Interestingly, by generating tri-valent constructs, having anti-MIF Nbs on the ends and an anti-albumin Nb in the middle, to increase the half-life, the TNF expression was further reduced. More importantly, the tri-valent constructs were shown to be protective in a murine endotoxemia model, increasing mice survival. Based on these results and taking into consideration MIF’s pro-tumoral role, we decided to test whether these constructs can reduce tumor growth as monotherapy or increase the efficacy of current immunotherapies, such as PD-1 antibodies. We found that the anti-MIF monotherapy significantly reduces tumor growth compared to the untreated and the anti-PD-1 treated groups. The group receiving anti-MIF + anti-PD-1 also showed a slower growth compared to the untreated group, and the anti-PD-1 group, however, there are no significant differences between the mono- and combinatorial treatment regarding tumor growth, suggesting no additional contribution of the anti-PD-1 treatment. Within the tumor microenvironment, we found a significant increase of CD45+cells, CD4+ T cells, and IFN-γ CD8+ producing cells in the anti-MIF + anti-PD-1 treated group compared to the other groups. As a next step, we will include models which are less responsive to immunotherapy, where new alternatives are highly needed.

AB - The macrophage migration inhibitory factor or MIF is a multifunctional cytokine that once bound to CD74, its main receptor, promotes the expression of pro-inflammatory cytokines, angiogenesis, and cell survival among other functions. MIF has been implicated as a biomarker of different diseases that have an inflammatory component, such as autoimmune diseases, metabolic disorders, systemic infections, and cancer. In this context, cross-reactive anti-MIF nanobodies (Nbs) were developed, and 11 different Nbs belonging to 7 different families were selected. We found that 2 out of the 11 Nbs significantly reduced TNF expression of murine and human LPS-stimulated cells. Interestingly, by generating tri-valent constructs, having anti-MIF Nbs on the ends and an anti-albumin Nb in the middle, to increase the half-life, the TNF expression was further reduced. More importantly, the tri-valent constructs were shown to be protective in a murine endotoxemia model, increasing mice survival. Based on these results and taking into consideration MIF’s pro-tumoral role, we decided to test whether these constructs can reduce tumor growth as monotherapy or increase the efficacy of current immunotherapies, such as PD-1 antibodies. We found that the anti-MIF monotherapy significantly reduces tumor growth compared to the untreated and the anti-PD-1 treated groups. The group receiving anti-MIF + anti-PD-1 also showed a slower growth compared to the untreated group, and the anti-PD-1 group, however, there are no significant differences between the mono- and combinatorial treatment regarding tumor growth, suggesting no additional contribution of the anti-PD-1 treatment. Within the tumor microenvironment, we found a significant increase of CD45+cells, CD4+ T cells, and IFN-γ CD8+ producing cells in the anti-MIF + anti-PD-1 treated group compared to the other groups. As a next step, we will include models which are less responsive to immunotherapy, where new alternatives are highly needed.

M3 - Poster

T2 - 35th Conference of the European Macrophage and Dendritic cell Society

Y2 - 19 September 2022 through 21 September 2022

ER -

Anti-MIF nanobodies as a novel tool to improve cancer therapy

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