Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles

Selina Lehrian; Anna Wasynczuk; Janina Petry; Melanie Guderian; Jan Nouta; Jana Sophia Buhre; Hanna B. Lunding; Philipp Köcher; Hannah Franziska Schumacher; Lara Dühring; Kathleen Kurwahn; Kristina Manzhula; Rudolf Manz; Yannic C. Bartsch; Manfred Wuhrer; Marc Ehlers

doi:10.1186/s40164-025-00708-6

Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles

Selina Lehrian, Anna Wasynczuk, Janina Petry, Melanie Guderian, Jan Nouta, Jana Sophia Buhre, Hanna B. Lunding, Philipp Köcher, Hannah Franziska Schumacher, Lara Dühring, Kathleen Kurwahn, Kristina Manzhula, Rudolf Manz, Yannic C. Bartsch, Manfred Wuhrer, Marc Ehlers^*

^*Korrespondierende/r Autor/-in für diese Arbeit

Abstract

Vaccination with tumor-(neo) antigen plus adjuvant is emerging as a promising cancer-therapy. However, as different adjuvants induce distinct immune cell and antibody (Ab) responses, selecting the right adjuvants remains challenging. Here, we evaluated the following vaccine adjuvants to promote protection against tumor-growth in mice and correlated IgG subclass and Fc N-glycosylation responses: Alum; the toll-like receptor activators Poly(I:C) and MPLA; Alum-Poly(I:C); and the more inflammatory water-in-oil adjuvants Montanide, IFA, CFA, and M.tb.-enriched (e)CFA. While Alum and Montanide failed to protect, MPLA and IFA tended to protect, and Poly(I:C), Alum-Poly(I:C), CFA, and eCFA significantly protected against tumor-growth. Across all adjuvants, tumor-protection correlated with the induction of highly activating IgG2(c/b) Abs and afucosylated (F0) IgG1 Abs, the latter showing up to 5% abundance. While all adjuvants transiently induced IgG1 F0 following initial immunization, Poly(I:C)- and eCFA-induced memory responses also generated IgG1 F0 after repeated antigen-exposure without adjuvants. Additionally, Poly(I:C)-induced tumor-protection was associated with high IgG2c/IgG1 ratios, high levels of IgG galactosylation and sialylation, and IFNγ-producing CD8 + Tc1-cells. Conversely, Ova-eCFA-induced tumor-protection was additionally associated with high levels of IgG across all subclasses, but low levels of galactosylation and sialylation, and CD8 + Tc17- and CD4 + Th17-cells. Accordingly, tumor protecting adjuvants may induce common but also different protecting programs. A tumor-antigen-specific IgG2a monoclonal (m)Ab protected against tumor-growth in both its de-galactosylated and galactosylated plus sialylated forms, suggesting common and possibly distinct protective mechanisms. Tumor-protection via serum transfer from Poly(I:C)-immunized mice depended more on NK-cells, whereas eCFA-induced and non-sialylated/non-galactosylated mAbs promoted neutrophil activation. These findings may help to improve tumor vaccination protocols.

Originalsprache	Englisch
Aufsatznummer	122
Zeitschrift	Experimental Hematology and Oncology
Jahrgang	14
Ausgabenummer	1
DOIs	https://doi.org/10.1186/s40164-025-00708-6
Publikationsstatus	Veröffentlicht - 12.2025

Fördermittel

Deutsche Forschungsgemeinschaft (German Research Foundation): Grants 429175970 (RTG 2633 “Defining and Targeting Autoimmune Pre-Disease”) and 390884018 (Germany's Excellence Strategies—EXC 2167, Precision Medicine in Chronic Inflammation (PMI)). JSB, PK and KM were PhD students and HFS was MD student of the RTG 2633. Federal Ministery of Education and Research, Germany: Grant 01KX2121 (NUM / COVIM 2.0).

Träger	Trägernummer
Deutsche Forschungsgemeinschaft	390884018, RTG 2633, 429175970
Bundesministerium für Bildung und Forschung	NUM / COVIM 2.0, 01KX2121

UN SDGs

Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 3 – Gesundheit und Wohlergehen

Strategische Forschungsbereiche und Zentren

Forschungsschwerpunkt: Infektion und Entzündung - Zentrum für Infektions- und Entzündungsforschung Lübeck (ZIEL)
Profilbereich: Lübeck Integrated Oncology Network (LION)

DFG-Fachsystematik

2.21-05 Immunologie
2.22-14 Hämatologie, Onkologie

Dokumente

10.1186/s40164-025-00708-6

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Lehrian, S., Wasynczuk, A., Petry, J., Guderian, M., Nouta, J., Buhre, J. S., Lunding, H. B., Köcher, P., Schumacher, H. F., Dühring, L., Kurwahn, K., Manzhula, K., Manz, R., Bartsch, Y. C., Wuhrer, M., & Ehlers, M. (2025). Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles. Experimental Hematology and Oncology, 14(1), Artikel 122. https://doi.org/10.1186/s40164-025-00708-6

@article{297b9a7189c44da0a65a6c33cd316602,

title = "Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles",

abstract = "Vaccination with tumor-(neo) antigen plus adjuvant is emerging as a promising cancer-therapy. However, as different adjuvants induce distinct immune cell and antibody (Ab) responses, selecting the right adjuvants remains challenging. Here, we evaluated the following vaccine adjuvants to promote protection against tumor-growth in mice and correlated IgG subclass and Fc N-glycosylation responses: Alum; the toll-like receptor activators Poly(I:C) and MPLA; Alum-Poly(I:C); and the more inflammatory water-in-oil adjuvants Montanide, IFA, CFA, and M.tb.-enriched (e)CFA. While Alum and Montanide failed to protect, MPLA and IFA tended to protect, and Poly(I:C), Alum-Poly(I:C), CFA, and eCFA significantly protected against tumor-growth. Across all adjuvants, tumor-protection correlated with the induction of highly activating IgG2(c/b) Abs and afucosylated (F0) IgG1 Abs, the latter showing up to 5\% abundance. While all adjuvants transiently induced IgG1 F0 following initial immunization, Poly(I:C)- and eCFA-induced memory responses also generated IgG1 F0 after repeated antigen-exposure without adjuvants. Additionally, Poly(I:C)-induced tumor-protection was associated with high IgG2c/IgG1 ratios, high levels of IgG galactosylation and sialylation, and IFNγ-producing CD8 + Tc1-cells. Conversely, Ova-eCFA-induced tumor-protection was additionally associated with high levels of IgG across all subclasses, but low levels of galactosylation and sialylation, and CD8 + Tc17- and CD4 + Th17-cells. Accordingly, tumor protecting adjuvants may induce common but also different protecting programs. A tumor-antigen-specific IgG2a monoclonal (m)Ab protected against tumor-growth in both its de-galactosylated and galactosylated plus sialylated forms, suggesting common and possibly distinct protective mechanisms. Tumor-protection via serum transfer from Poly(I:C)-immunized mice depended more on NK-cells, whereas eCFA-induced and non-sialylated/non-galactosylated mAbs promoted neutrophil activation. These findings may help to improve tumor vaccination protocols.",

author = "Selina Lehrian and Anna Wasynczuk and Janina Petry and Melanie Guderian and Jan Nouta and Buhre, \{Jana Sophia\} and Lunding, \{Hanna B.\} and Philipp K{\"o}cher and Schumacher, \{Hannah Franziska\} and Lara D{\"u}hring and Kathleen Kurwahn and Kristina Manzhula and Rudolf Manz and Bartsch, \{Yannic C.\} and Manfred Wuhrer and Marc Ehlers",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = dec,

doi = "10.1186/s40164-025-00708-6",

language = "English",

volume = "14",

journal = "Experimental Hematology and Oncology",

issn = "2162-3619",

publisher = "BioMed Central Ltd",

number = "1",

}

Lehrian, S, Wasynczuk, A, Petry, J, Guderian, M, Nouta, J, Buhre, JS, Lunding, HB, Köcher, P, Schumacher, HF, Dühring, L, Kurwahn, K, Manzhula, K , Manz, R, Bartsch, YC, Wuhrer, M & Ehlers, M 2025, 'Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles', Experimental Hematology and Oncology, Jg. 14, Nr. 1, 122. https://doi.org/10.1186/s40164-025-00708-6

TY - JOUR

T1 - Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles

AU - Lehrian, Selina

AU - Wasynczuk, Anna

AU - Petry, Janina

AU - Guderian, Melanie

AU - Nouta, Jan

AU - Buhre, Jana Sophia

AU - Lunding, Hanna B.

AU - Köcher, Philipp

AU - Schumacher, Hannah Franziska

AU - Dühring, Lara

AU - Kurwahn, Kathleen

AU - Manzhula, Kristina

AU - Manz, Rudolf

AU - Bartsch, Yannic C.

AU - Wuhrer, Manfred

AU - Ehlers, Marc

PY - 2025/12

Y1 - 2025/12

N2 - Vaccination with tumor-(neo) antigen plus adjuvant is emerging as a promising cancer-therapy. However, as different adjuvants induce distinct immune cell and antibody (Ab) responses, selecting the right adjuvants remains challenging. Here, we evaluated the following vaccine adjuvants to promote protection against tumor-growth in mice and correlated IgG subclass and Fc N-glycosylation responses: Alum; the toll-like receptor activators Poly(I:C) and MPLA; Alum-Poly(I:C); and the more inflammatory water-in-oil adjuvants Montanide, IFA, CFA, and M.tb.-enriched (e)CFA. While Alum and Montanide failed to protect, MPLA and IFA tended to protect, and Poly(I:C), Alum-Poly(I:C), CFA, and eCFA significantly protected against tumor-growth. Across all adjuvants, tumor-protection correlated with the induction of highly activating IgG2(c/b) Abs and afucosylated (F0) IgG1 Abs, the latter showing up to 5% abundance. While all adjuvants transiently induced IgG1 F0 following initial immunization, Poly(I:C)- and eCFA-induced memory responses also generated IgG1 F0 after repeated antigen-exposure without adjuvants. Additionally, Poly(I:C)-induced tumor-protection was associated with high IgG2c/IgG1 ratios, high levels of IgG galactosylation and sialylation, and IFNγ-producing CD8 + Tc1-cells. Conversely, Ova-eCFA-induced tumor-protection was additionally associated with high levels of IgG across all subclasses, but low levels of galactosylation and sialylation, and CD8 + Tc17- and CD4 + Th17-cells. Accordingly, tumor protecting adjuvants may induce common but also different protecting programs. A tumor-antigen-specific IgG2a monoclonal (m)Ab protected against tumor-growth in both its de-galactosylated and galactosylated plus sialylated forms, suggesting common and possibly distinct protective mechanisms. Tumor-protection via serum transfer from Poly(I:C)-immunized mice depended more on NK-cells, whereas eCFA-induced and non-sialylated/non-galactosylated mAbs promoted neutrophil activation. These findings may help to improve tumor vaccination protocols.

AB - Vaccination with tumor-(neo) antigen plus adjuvant is emerging as a promising cancer-therapy. However, as different adjuvants induce distinct immune cell and antibody (Ab) responses, selecting the right adjuvants remains challenging. Here, we evaluated the following vaccine adjuvants to promote protection against tumor-growth in mice and correlated IgG subclass and Fc N-glycosylation responses: Alum; the toll-like receptor activators Poly(I:C) and MPLA; Alum-Poly(I:C); and the more inflammatory water-in-oil adjuvants Montanide, IFA, CFA, and M.tb.-enriched (e)CFA. While Alum and Montanide failed to protect, MPLA and IFA tended to protect, and Poly(I:C), Alum-Poly(I:C), CFA, and eCFA significantly protected against tumor-growth. Across all adjuvants, tumor-protection correlated with the induction of highly activating IgG2(c/b) Abs and afucosylated (F0) IgG1 Abs, the latter showing up to 5% abundance. While all adjuvants transiently induced IgG1 F0 following initial immunization, Poly(I:C)- and eCFA-induced memory responses also generated IgG1 F0 after repeated antigen-exposure without adjuvants. Additionally, Poly(I:C)-induced tumor-protection was associated with high IgG2c/IgG1 ratios, high levels of IgG galactosylation and sialylation, and IFNγ-producing CD8 + Tc1-cells. Conversely, Ova-eCFA-induced tumor-protection was additionally associated with high levels of IgG across all subclasses, but low levels of galactosylation and sialylation, and CD8 + Tc17- and CD4 + Th17-cells. Accordingly, tumor protecting adjuvants may induce common but also different protecting programs. A tumor-antigen-specific IgG2a monoclonal (m)Ab protected against tumor-growth in both its de-galactosylated and galactosylated plus sialylated forms, suggesting common and possibly distinct protective mechanisms. Tumor-protection via serum transfer from Poly(I:C)-immunized mice depended more on NK-cells, whereas eCFA-induced and non-sialylated/non-galactosylated mAbs promoted neutrophil activation. These findings may help to improve tumor vaccination protocols.

UR - https://www.scopus.com/pages/publications/105018198613

U2 - 10.1186/s40164-025-00708-6

DO - 10.1186/s40164-025-00708-6

M3 - Letters

AN - SCOPUS:105018198613

SN - 2162-3619

VL - 14

JO - Experimental Hematology and Oncology

JF - Experimental Hematology and Oncology

IS - 1

M1 - 122

ER -

Anti-tumor vaccine efficacy depends on adjuvant type and associates with induced IgG subclass and glycosylation profiles

Abstract

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