Nipocalimab, an immunoselective FcRn blocker that lowers IgG and has unique molecular properties.

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Tác giả: Katie Abouzahr, William Avery, Traymon Beavers, Sayak Bhattacharya, Julia Brown, Hsin Chen, Amit Choudhury, Edward Cochran, Thomas Daly, Jay Duffner, Matthew DuPrie, Fiona Elwood, Jonathan J Hubbard, Sujatha Kumar, Leona E Ling, Lynn Markowitz, James Meador, Pushpa Narayanaswami, Yvonne Pao, Viraj Parge, Karen Price, Sucharita Roy, Laura Rutitzky, Nilufer P Seth, Samuel Sihapong, Siddharth Sukumaran, Steven Tyler, Yang Wang, Rui Xu

Ngôn ngữ: eng

Ký hiệu phân loại: 497.52539 Siouan, lroquian, Hokan, Chumash, Yuki languages

Thông tin xuất bản: United States : mAbs , 2025

Mô tả vật lý:

Bộ sưu tập: NCBI

ID: 194654

Nipocalimab is a human immunoglobulin G (IgG)1 monoclonal antibody that binds to the neonatal Fc receptor (FcRn) with high specificity and high affinity at both neutral (extracellular) and acidic (intracellular) pH, resulting in the reduction of circulating IgG levels, including those of pathogenic IgG antibodies. Here, we present the molecular, cellular, and nonclinical characteristics of nipocalimab that support the reported clinical pharmacology and potential clinical application in IgG-driven, autoantibody- and alloantibody-mediated diseases. The crystal structure of the nipocalimab antigen binding fragment (Fab)/FcRn complex reveals its binding to a unique epitope on the IgG binding site of FcRn that supports the observed pH-independent high-binding affinity to FcRn. Cell-based and in vivo studies demonstrate concentration/dose- and time-dependent FcRn occupancy and IgG reduction. Nipocalimab selectively reduces circulating IgG levels without detectable effects on other adaptive and innate immune functions. In vitro experiments and in vivo studies in mice and cynomolgus monkeys generated data that align with observations from clinical studies of nipocalimab in IgG autoantibody- and alloantibody-mediated diseases.
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