What question did this study set out to answer?

The aim is to explore the cellular targets and systemic regulatory effects of polyvalent IgG.

June 1, 2026Open Access

System-wide immunoregulation by polyvalent IgG: integrating transcriptomic, miRNA, and proteomic landscapes

Key Points

The aim is to explore the cellular targets and systemic regulatory effects of polyvalent IgG.
PBMCs from 20 healthy donors were cultured with polyvalent IgG for 72 hours.
Cell viability and immune markers were assessed using flow cytometry, RNA-seq, and proteomics.
Pathogen-derived epitope recognition was analyzed with a microarray.
pIgG preserved PBMC viability and reduced IL-17⁺ CD4⁺ T cells (significant change), and increased IL-10⁺ B cells.
Transcriptomic analysis revealed 4,820 upregulated genes and enrichment in MHC class II pathways.
Proteome profiling identified ~130 IgG-recognized proteins and 948 pathogen sequences from various microorganisms.

Abstract

Abstract Background Polyvalent IgG (pIgG/IVIg), derived from thousands of donors, exerts broad immunomodulatory effects; however, its direct cellular targets and genome-wide regulatory impacts remain incompletely defined. Methods Peripheral blood mononuclear cells (PBMCs) from 20 healthy donors were cultured for 72 h with pIgG (100 µg/mL) or mock conditions. Cell viability, phenotype, memory subsets, chemokine receptors, and intracellular cytokines were assessed by flow cytometry. Differential gene expression, miRNA/sRNA profiles, and pathway enrichments were analyzed by RNA-seq and small-RNA sequencing. Proteome-wide IgG binding was mapped using human proteome microarrays across lymphoid subsets, and pathogen-derived linear epitope recognition was evaluated using a 4,345-epitope infectious-disease microarray. Results pIgG preserved PBMC viability but significantly modulated immune function: it reduced IL-17⁺ CD4⁺ T cells and tissue-resident memory T cells, decreased IL-4⁺ CD8⁺ T cells, enhanced IFN-γ⁺ γδ T cells, downregulated CCR5 and CCR6, and expanded IL-10⁺ B cells while reducing IL-13⁺ and IL-17⁺ B cells. Transcriptomic analysis revealed 4,820 upregulated and 2,160 downregulated genes, with enrichment of MHC class II and TCR-signaling pathways and selective modulation of cytokine, chemokine, CD, and HLA genes. Innate sensors—including TLR4, TLR8, and NLR4—were downregulated. Small-RNA analysis identified 19 differentially expressed miRNAs and 79 novel sRNAs, indicating epigenetic remodeling. Proteome-wide profiling detected ~ 130 IgG-recognized proteins per lymphocyte subset and 180 shared targets enriched in cytosolic, vesicular, and endocytic pathways. Pathogen-epitope profiling identified 948 recognized sequences from 56 viruses, 21 bacteria, and 12 parasites. Conclusions pIgG functions as a multilayered immunoregulator that attenuates Th17-associated inflammation, promotes IL-10–mediated regulatory circuits, and modulates receptor signaling and antigen-processing pathways. These findings underscore its potential for broad therapeutic immunomodulation.

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System-wide immunoregulation by polyvalent IgG: integrating transcriptomic, miRNA, and proteomic landscapes

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Abstract

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