Immunological and physical evaluation of the multistage tuberculosis subunit vaccine candidate H56/CAF01 formulated as a spray-dried powder

Aneesh Thakur; Pall Thor Ingvarsson; Signe Tandrup Schmidt; Fabrice Rose; Peter Andersen; Dennis Christensen; Camilla Foged

doi:10.1016/j.vaccine.2018.04.055

Immunological and physical evaluation of the multistage tuberculosis subunit vaccine candidate H56/CAF01 formulated as a spray-dried powder

Aneesh Thakur
, Pall Thor Ingvarsson
, Signe Tandrup Schmidt
, Fabrice Rose
, Peter Andersen
, Dennis Christensen
, Camilla Foged

Faculty of Pharmaceutical Sciences

University of Iceland

Research output: Contribution to journal › Article › peer-review

Abstract

Liquid vaccine dosage forms have limited stability and require refrigeration during their manufacture, distribution and storage. In contrast, solid vaccine dosage forms, produced by for example spray drying, offer improved storage stability and reduced dependence on cold-chain facilities. This is advantageous for mass immunization campaigns for global public health threats, e.g., tuberculosis (TB), and offers cheaper vaccine distribution. The multistage subunit vaccine antigen H56, which is a fusion protein of the Mycobacterium tuberculosis (Mtb) antigens Ag85B, ESAT-6, and Rv2660, has been shown to confer protective efficacy against active TB before and after Mtb exposure in preclinical models, and it is currently undergoing clinical phase 2a testing. In several studies, including a recent study comparing multiple clinically relevant vaccine adjuvants, the T helper type 1 (Th1)/Th17-inducing adjuvant CAF01 was the most efficacious adjuvant for H56 to stimulate protective immunity against Mtb. With the long-term goal of designing a thermostable and self-administrable dry powder vaccine based on H56 and CAF01 for inhalation, we compared H56 spray-dried with CAF01 with the non-spray-dried H56/CAF01 vaccine with respect to their ability to induce systemic Th1, Th17 and humoral responses after subcutaneous immunization. Here we show that spray drying of the H56/CAF01 vaccine results in preserved antigenic epitope recognition and adjuvant activity of CAF01, and the spray-dried, reconstituted vaccine induces antigen-specific Th1, Th17 and humoral immune responses, which are comparable to those stimulated by the non-spray-dried H56/CAF01 vaccine. In addition, the spray-dried and reconstituted H56/CAF01 vaccine promotes similar polyfunctional CD4⁺ T-cell responses as the non-spray-dried vaccine. Thus, our study provides proof-of-concept that spray drying of the subunit vaccine H56/CAF01 preserves vaccine-induced humoral and cell-mediated immune responses. These results support our ongoing efforts to develop a thermostable, dry powder-based TB vaccine.

Original language	English
Pages (from-to)	3331-3339
Number of pages	9
Journal	Vaccine
Volume	36
Issue number	23
DOIs	https://doi.org/10.1016/j.vaccine.2018.04.055
Publication status	Published - 31 May 2018

Bibliographical note

Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052)], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422) and the European Union's H2020 Programme “TBVAC2020” (grant number 643381). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052 )], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422 ) and the European Union’s H2020 Programme “TBVAC2020” (grant number 643381 ). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Publisher Copyright: © 2018 Elsevier Ltd

Other keywords

CAF01
H56
Spray drying
Th1/Th17
Tuberculosis
Vaccine

Access to Document

10.1016/j.vaccine.2018.04.055

Cite this

@article{44a8828db79c49af966c6c923dbc3694,

title = "Immunological and physical evaluation of the multistage tuberculosis subunit vaccine candidate H56/CAF01 formulated as a spray-dried powder",

abstract = "Liquid vaccine dosage forms have limited stability and require refrigeration during their manufacture, distribution and storage. In contrast, solid vaccine dosage forms, produced by for example spray drying, offer improved storage stability and reduced dependence on cold-chain facilities. This is advantageous for mass immunization campaigns for global public health threats, e.g., tuberculosis (TB), and offers cheaper vaccine distribution. The multistage subunit vaccine antigen H56, which is a fusion protein of the Mycobacterium tuberculosis (Mtb) antigens Ag85B, ESAT-6, and Rv2660, has been shown to confer protective efficacy against active TB before and after Mtb exposure in preclinical models, and it is currently undergoing clinical phase 2a testing. In several studies, including a recent study comparing multiple clinically relevant vaccine adjuvants, the T helper type 1 (Th1)/Th17-inducing adjuvant CAF01 was the most efficacious adjuvant for H56 to stimulate protective immunity against Mtb. With the long-term goal of designing a thermostable and self-administrable dry powder vaccine based on H56 and CAF01 for inhalation, we compared H56 spray-dried with CAF01 with the non-spray-dried H56/CAF01 vaccine with respect to their ability to induce systemic Th1, Th17 and humoral responses after subcutaneous immunization. Here we show that spray drying of the H56/CAF01 vaccine results in preserved antigenic epitope recognition and adjuvant activity of CAF01, and the spray-dried, reconstituted vaccine induces antigen-specific Th1, Th17 and humoral immune responses, which are comparable to those stimulated by the non-spray-dried H56/CAF01 vaccine. In addition, the spray-dried and reconstituted H56/CAF01 vaccine promotes similar polyfunctional CD4+ T-cell responses as the non-spray-dried vaccine. Thus, our study provides proof-of-concept that spray drying of the subunit vaccine H56/CAF01 preserves vaccine-induced humoral and cell-mediated immune responses. These results support our ongoing efforts to develop a thermostable, dry powder-based TB vaccine.",

keywords = "CAF01, H56, Spray drying, Th1/Th17, Tuberculosis, Vaccine",

author = "Aneesh Thakur and Ingvarsson, \{Pall Thor\} and Schmidt, \{Signe Tandrup\} and Fabrice Rose and Peter Andersen and Dennis Christensen and Camilla Foged",

note = "Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052)], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422) and the European Union's H2020 Programme “TBVAC2020” (grant number 643381). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052 )], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422 ) and the European Union{\textquoteright}s H2020 Programme “TBVAC2020” (grant number 643381 ). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Publisher Copyright: {\textcopyright} 2018 Elsevier Ltd",

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doi = "10.1016/j.vaccine.2018.04.055",

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T1 - Immunological and physical evaluation of the multistage tuberculosis subunit vaccine candidate H56/CAF01 formulated as a spray-dried powder

AU - Thakur, Aneesh

AU - Ingvarsson, Pall Thor

AU - Schmidt, Signe Tandrup

AU - Rose, Fabrice

AU - Andersen, Peter

AU - Christensen, Dennis

AU - Foged, Camilla

N1 - Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052)], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422) and the European Union's H2020 Programme “TBVAC2020” (grant number 643381). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Funding Information: This study was supported by Innovation Fund Denmark [previously the Danish Strategic Research Council (grant number 09-067052 )], The Danish Council for Independent Research, Technology and Production Sciences (grant number DFF-4184-00422 ) and the European Union’s H2020 Programme “TBVAC2020” (grant number 643381 ). We are grateful to the animal care staff at Statens Serum Institut for excellent technical assistance. Publisher Copyright: © 2018 Elsevier Ltd

PY - 2018/5/31

Y1 - 2018/5/31

N2 - Liquid vaccine dosage forms have limited stability and require refrigeration during their manufacture, distribution and storage. In contrast, solid vaccine dosage forms, produced by for example spray drying, offer improved storage stability and reduced dependence on cold-chain facilities. This is advantageous for mass immunization campaigns for global public health threats, e.g., tuberculosis (TB), and offers cheaper vaccine distribution. The multistage subunit vaccine antigen H56, which is a fusion protein of the Mycobacterium tuberculosis (Mtb) antigens Ag85B, ESAT-6, and Rv2660, has been shown to confer protective efficacy against active TB before and after Mtb exposure in preclinical models, and it is currently undergoing clinical phase 2a testing. In several studies, including a recent study comparing multiple clinically relevant vaccine adjuvants, the T helper type 1 (Th1)/Th17-inducing adjuvant CAF01 was the most efficacious adjuvant for H56 to stimulate protective immunity against Mtb. With the long-term goal of designing a thermostable and self-administrable dry powder vaccine based on H56 and CAF01 for inhalation, we compared H56 spray-dried with CAF01 with the non-spray-dried H56/CAF01 vaccine with respect to their ability to induce systemic Th1, Th17 and humoral responses after subcutaneous immunization. Here we show that spray drying of the H56/CAF01 vaccine results in preserved antigenic epitope recognition and adjuvant activity of CAF01, and the spray-dried, reconstituted vaccine induces antigen-specific Th1, Th17 and humoral immune responses, which are comparable to those stimulated by the non-spray-dried H56/CAF01 vaccine. In addition, the spray-dried and reconstituted H56/CAF01 vaccine promotes similar polyfunctional CD4+ T-cell responses as the non-spray-dried vaccine. Thus, our study provides proof-of-concept that spray drying of the subunit vaccine H56/CAF01 preserves vaccine-induced humoral and cell-mediated immune responses. These results support our ongoing efforts to develop a thermostable, dry powder-based TB vaccine.

AB - Liquid vaccine dosage forms have limited stability and require refrigeration during their manufacture, distribution and storage. In contrast, solid vaccine dosage forms, produced by for example spray drying, offer improved storage stability and reduced dependence on cold-chain facilities. This is advantageous for mass immunization campaigns for global public health threats, e.g., tuberculosis (TB), and offers cheaper vaccine distribution. The multistage subunit vaccine antigen H56, which is a fusion protein of the Mycobacterium tuberculosis (Mtb) antigens Ag85B, ESAT-6, and Rv2660, has been shown to confer protective efficacy against active TB before and after Mtb exposure in preclinical models, and it is currently undergoing clinical phase 2a testing. In several studies, including a recent study comparing multiple clinically relevant vaccine adjuvants, the T helper type 1 (Th1)/Th17-inducing adjuvant CAF01 was the most efficacious adjuvant for H56 to stimulate protective immunity against Mtb. With the long-term goal of designing a thermostable and self-administrable dry powder vaccine based on H56 and CAF01 for inhalation, we compared H56 spray-dried with CAF01 with the non-spray-dried H56/CAF01 vaccine with respect to their ability to induce systemic Th1, Th17 and humoral responses after subcutaneous immunization. Here we show that spray drying of the H56/CAF01 vaccine results in preserved antigenic epitope recognition and adjuvant activity of CAF01, and the spray-dried, reconstituted vaccine induces antigen-specific Th1, Th17 and humoral immune responses, which are comparable to those stimulated by the non-spray-dried H56/CAF01 vaccine. In addition, the spray-dried and reconstituted H56/CAF01 vaccine promotes similar polyfunctional CD4+ T-cell responses as the non-spray-dried vaccine. Thus, our study provides proof-of-concept that spray drying of the subunit vaccine H56/CAF01 preserves vaccine-induced humoral and cell-mediated immune responses. These results support our ongoing efforts to develop a thermostable, dry powder-based TB vaccine.

KW - CAF01

KW - H56

KW - Spray drying

KW - Th1/Th17

KW - Tuberculosis

KW - Vaccine

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M3 - Article

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JO - Vaccine

JF - Vaccine

IS - 23

ER -

Immunological and physical evaluation of the multistage tuberculosis subunit vaccine candidate H56/CAF01 formulated as a spray-dried powder

Abstract

Bibliographical note

Other keywords

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