859 Tuning the tumor microenvironment by reprogramming TREM1+ myeloid cells to unleash anti-tumor immunity in solid tumors

Jahchan, Nadine S.; Ramoth, Hanna; Juric, Vladi; Mayes, Erin; Mankikar, Shilpa; Mehta, Ranna; Dash, Subhadra; Palmer, Rachael; Pollack, Joshua L.; Rudolph, Joshua; Canaday, Pamela S.; Haeggblom, Linnea; Santamaría, Carlos; Du, Xiaoyan; Reyno, Leonard; Baker, Kevin P.; Liang, Linda

doi:10.1136/jitc-2021-sitc2021.859

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“…Following complete eradication of the tumour, scarring often occurs at the site of tumour implantation, leaving behind connective tissue that may be mistaken for a small tumour; thus, tumour width or length below the limit of detection (4 mm) resulting in tumour volume of 32 mm 3 was selected as the cut-off for complete tumour regression at the end of the simulation (960 h). The chosen cut-off for complete response (tumour volume ≤ 32 mm 3 ) is in line with reported values [ 56 , 57 , 58 ]. TGI model parameters for simulations of tumour volume at HEDs for studied compounds after 1 or 2 cycles of therapy are summarised in Tables S15–S17 .…”

Section: Methodsmentioning

confidence: 64%

In Vitro/In Vivo Translation of Synergistic Combination of MDM2 and MEK Inhibitors in Melanoma Using PBPK/PD Modelling: Part II

Witkowski

Polak

Rogulski

et al. 2022

IJMS

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The development of in vitro/in vivo translational methods for synergistically acting drug combinations is needed to identify the most effective therapeutic strategies. We performed PBPK/PD modelling for siremadlin, trametinib, and their combination at various dose levels and dosing schedules in an A375 xenografted mouse model (melanoma cells). In this study, we built models based on in vitro ADME and in vivo PK/PD data determined from the literature or estimated by the Simcyp Animal simulator (V21). The developed PBPK/PD models allowed us to account for the interactions between siremadlin and trametinib at PK and PD levels. The interaction at the PK level was described by an interplay between absorption and tumour disposition levels, whereas the PD interaction was based on the in vitro results. This approach allowed us to reasonably estimate the most synergistic and efficacious dosing schedules and dose levels for combinations of siremadlin and trametinib in mice. PBPK/PD modelling is a powerful tool that allows researchers to properly estimate the in vivo efficacy of the anticancer drug combination based on the results of in vitro studies. Such an approach based on in vitro and in vivo extrapolation may help researchers determine the most efficacious dosing strategies and will allow for the extrapolation of animal PBPK/PD models into clinical settings.

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Section: Methodsmentioning

confidence: 64%