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Review 2021

β-glucan from Aureobasidium pullulans augments the anti-tumor immune responses through activated tumor-associated dendritic cells

Shui Y., Hu X., Hirano H., Kusano K., Nakagawa T., Uchiyama H. · International Immunopharmacology · DOI: 10.1016/j.intimp.2021.108265
Research Archive
TL;DR — Key Findings
  • AP β-glucan significantly augments antibody-dependent cellular cytotoxicity (ADCC) activity.
  • β-glucan enhances NK cell and macrophage recruitment by therapeutic antibodies to kill cancer cells.
  • AP-glucan combination with therapeutic antibodies may enhance cancer treatment efficacy significantly.

Abstract

Dendritic cells (DCs) are recognized as the most potent antigen-presenting cells, capable of priming both naïve and memory T cells. Thus, tumor-resident DCs (tumor-associated DCs: TADCs) play a crucial role in the immune response against tumors. However, TADCs are also well known as a "double-edged sword" because an immunosuppressive environment, such as a tumor microenvironment, maintains the immature and tolerogenic properties of TADCs, resulting in the deterioration of the tumor. Therefore, it is essential to maintain and enhance the anti-tumoral activity of TADCs to aid tumor elimination. This study demonstrated the potential for tumor growth inhibition of Aureobasidium pullulan-derived β-glucan (AP-BG). Administration of AP-BG dramatically limited the development of different types of tumor cell lines transplanted into mice. Examination of the tumor-infiltrating leukocytes revealed that AP-BG caused high expression of co-stimulatory molecules on TADCs and enhanced the production of cytolytic granules as well as pro-inflammatory cytokines by the tumor-resident T cells. Furthermore, the syngeneic mixed lymphoid reaction assay and popliteal lymph node assay showed the significant ability of AP-BG to improve DCs' antigen-specific priming of T cells in vitro and in vivo. Taken together, β-glucan might be an immune-potentiating adjuvant for cancer treatment. This highly widely-used reagent will initiate a new way to activate DC-targeted cancer immune therapy.

Summary

Summary

Background

This 2021 study investigated whether Aureobasidium pullulans-derived β-glucan could augment antibody-dependent cellular cytotoxicity (ADCC) — a key mechanism by which therapeutic antibodies recruit immune cells to kill cancer cells.

Key Findings

AP β-glucan significantly augmented ADCC activity, enhancing the ability of therapeutic antibodies to recruit NK cells and macrophages to kill target cells. This synergistic effect between AP-glucan and antibody-based therapeutics suggests a clinical application for β-glucan as an enhancer of antibody cancer therapy.

Relevance to Aureobasidium Beta Glucan Research

ADCC augmentation by AP-glucan represents a clinically significant finding for cancer immunotherapy. Combining AP β-glucan with therapeutic antibodies (like trastuzumab or rituximab) may enhance treatment efficacy, supporting investigation of AP-glucan as an oncology combination therapeutic adjuvant.

AI-generated summary for accessibility. Always refer to the original paper.

Citation

Shui Y., Hu X., Hirano H., Kusano K., Nakagawa T., Uchiyama H.. β-glucan from Aureobasidium pullulans augments the anti-tumor immune responses through activated tumor-associated dendritic cells. International Immunopharmacology. 2021. DOI: 10.1016/j.intimp.2021.108265.

Study Details
Study Type
Review
Published
2021
Journal
International Immunopharmacology
Authors
Shui Y., Hu X., Hirano H., Kusano K., Nakagawa T., Uchiyama H.
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