Journal: Molecular cancer
Article Title: Biologically targeted dual adaptive and innate nano-Immunotherapy for clear cell renal cell carcinoma treatment.
doi: 10.1186/s12943-025-02382-y
Figure Lengend Snippet: Fig. 8 The MINP platform reduces hepatotoxicity induced by agonistic α-4-1BB and α-CD25 antibodies in healthy immunocompetent mice. (A) Serum ALT, AST, and BUN levels recorded for healthy BALB/c mice 48 h after 4 i.v. administrations of free α-CA-9, α-4-1BB, and α-CD27, or α-CA-9/α-4-1BB/α- CD27 NPs (chimeric MINPs) (n = 7, except for mice treated with MINPs, where n = 8). (B) Representative H&E-stained images of the liver, lung, spleen, and kidney preserved from mice at the study endpoint. (C) Representative immunohistochemistry images of liver sections preserved at the study endpoint after different treatments. (D) Serum DyLight 650 fluorescent intensity 6 h after i.v. administration of DyLight 650 labeled α-CA-9, α-4-1BB, and α-CD27 or α-CA-9/α-4-1BB/α-CD27 NPs (functionalized with DyLight 650-labeled antibodies) (n = 5, except for the non-treatment control group, where n = 3). The chimeric MINPs were functionalized using anti-human CA-9, anti-mouse 4-1BB, and CD27 agonistic antibodies in these in vivo studies. Data are presented as mean ± SEM. All p-values were analyzed using two-way ANOVA with Tukey’s HSD multiple comparisons post-hoc test
Article Snippet: The actual degree of DBCOfunctionalization was calculated via UV-visible absorption spectroscopy using a DBCO absorption coefficient of 12,000 M− 1 L cm− 1 at 310 nm, an immunoglobulin absorption coefficient of 1.33 mg/mL cm− 1 at 280 nm for the anti-mouse 4-1BB and anti-mouse CD27 antibodies (as provided by BioXCell), 1.45 mg/mL cm− 1 for Girentuximab (anti-human CA-9), 1.66 mg/mL cm− 1 for Utomilumab (anti-human 4-1BB), and 1.61 mg/mL cm− 1 for Varlilumab (anti-human CD27), with a correction factor of 1.089 at 280 nm.
Techniques: Staining, Immunohistochemistry, Labeling, Control, In Vivo