NVL-520

NVL-520 : Inhibitor of ROS1 and ROS1 G2032R

Structure

Information

  • ROS1 (Mutant:WT, G2032R)
  • Inhibitor
  • up to 300 nM

In Vitro Validations

Uniprot ID: P08922
Target Class: Kinase
Target SubClass: TK
Potency: IC50
Potency Value: 0.7 nM
Potency Assay: Biochemical assay using WT ROS1
PDB ID for probe-target interaction (3D structure): 9QEK
Target aliases:
Proto-oncogene tyrosine-protein kinase ROS, ROS, M ...

DOI Reference: 10.1158/2159-8290.CD-22-0968

Uniprot ID: P08922
Target Class: Kinase
Target SubClass: TK
Potency: IC50
Potency Value: 7.9 nM
Potency Assay: Biochemical assay using ROS1 G2032R
PDB ID for probe-target interaction (3D structure): --
Target aliases:
Proto-oncogene tyrosine-protein kinase ROS, ROS, M ...

DOI Reference: 10.1158/2159-8290.CD-22-0968

In Cell Validations

In Vivo Data

Off-Target Selectivity Assesments

Probe Selectivity in Vitro:
In a biochemical screen against 335 wild-type human kinase domains, NVL-520 was highly selective. ROS1 was the most strongly inhibited target, followed by ALK which had 2-fold weaker IC50 than ROS1. Besides ALK, no other kinases were inhibited within 10-fold of the IC50 of NVL-520 for ROS1. NVL-520 had a >50-fold selectivity for ROS1 over 97.9% (328/335) of the tested kinome, with only five additional targets (LTK, FAK, PYK2, FER, and TRKB) inhibited with IC50 between 10- and 50-fold of ROS1. Because TRKB scored in this assay as a weak hit (IC50 = 28-fold above ROS1) and was a key off-target of concern, we further profiled TRKB using additional assays. NVL-520 demonstrated selectivity for both wild-type ROS1 and ROS1 G2032R over TRK (185-fold and 16-fold, respectively;
Probe Selectivity in Cell:
Selectivity against TRK family was confirmed via cell viability assay
Potency assay (off target): Mutagenesis screens: Predicting resistance in a TKI-naïve setting
Probe Selectivity in Vitro:
Zidesamtinib suppressed ROS1 mutations in ENU mutagenesis screens. (DOI: 10.1158/1535-7163.MCT-25-0025)
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