Pharmacokinetic evaluation of the PNC disassembler metarrestin in wild-type and Pdx1-Cre;LSL-KrasG12D/+;Tp53R172H/+ (KPC) mice, a genetically engineered model of pancreatic cancer.

Tomas Vilimas,Amy Wang,Samarjit Patnaik,Emma Hughes,Marc D. Singleton,Zachary Knotts,Dandan Li,Kevin J. Frankowski,Jerome J. Schlomer,Theresa M. Guerin,Stephanie Springer,Catherine Drennan,Christopher Dextras,Chen Wang,Debra Gilbert,Noel Southall,Marc Ferrer,Sui Huang,Serguei Kozlov,Juan J. Marugan,Xin Xu,Udo Rudloff

Pharmacokinetic evaluation of the PNC disassembler metarrestin in wild-type and Pdx1-Cre;LSL-KrasG12D/+;Tp53R172H/+ (KPC) mice, a genetically engineered model of pancreatic cancer.

2018

Purpose Metarrestin is a first-in-class small molecule clinical candidate capable of disrupting the perinucleolar compartment, a subnuclear structure unique to metastatic cancer cells. This study aims to define the pharmacokinetic (PK) profile of metarrestin and the pharmacokinetic/pharmacodynamic relationship of metarrestin-regulated markers.

Keywords:

Small molecule
Cancer cell
Disassembler
Perinucleolar compartment
Pharmacology
Wild type
Pancreatic cancer
PDX1
Medicine
Pharmacokinetics
Pharmacodynamics
Cmax
Volume of distribution
Bioavailability

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