PT - JOURNAL ARTICLE AU - JAEHYUN LEE AU - DONGGEON KIM AU - EUNJU SON AU - SU-JI YOO AU - JASON K. SA AU - YONG JAE SHIN AU - YEUP YOON AU - DO-HYUN NAM TI - Pharmacokinetics, Biodistribution, and Toxicity Evaluation of Anti-SEMA3A (F11) in <em>In Vivo</em> Models DP - 2018 May 01 TA - Anticancer Research PG - 2803--2810 VI - 38 IP - 5 4099 - http://ar.iiarjournals.org/content/38/5/2803.short 4100 - http://ar.iiarjournals.org/content/38/5/2803.full SO - Anticancer Res2018 May 01; 38 AB - Background/Aim: The aim of our study was to investigate the pharmacokinetics (PK), tissue distribution and toxicity of F11 antibody to semaphorin 3A in mouse models and explore its anti-angiogenic and tumor-inhibitory effect. Materials and Methods: Patient-derived xenograft (PDX) models were established via subcutaneous implantation of glioblastoma multiforme (GBM) cells and treated with F11. Results: F11 significantly attenuated tumor growth and angiogenesis in the GBM PDX model. Within the range of administered doses, the PK of F11 in serum demonstrated a linear fashion, consistent with general PK profiles of soluble antigen-targeting antibodies. Additionally, the clearance level was detected at between 4.63 and 7.12 ml/d/kg, while the biological half-life was measured at 6.9 and 9.4 days. Tissue distribution of F11 in kidney, liver and heart was consistent with previously reported antibody patterns. However, the presence of F11 in the brain was an interesting finding. Conclusion: Collectively, our results revealed angiogenic and tumor-inhibitory effect of F11 antibody and its potential therapeutic use within a clinical framework based on PK, biodistribution and toxicity evaluation in mouse models.