ISDA: 9DM8

Deposition Date 2024-09-12

Release Date 2026-01-28

Last Version Date 2026-02-25

Entry Detail

PDB ID:

9DM8

Keywords:

TRANSFERASE

Title:

EGFR wildtype in complex with BI-8128

Biological Source:

Source Organism(s):

Homo sapiens (Taxon ID: 9606)

Expression System(s):

Spodoptera frugiperda

Method Details:

Experimental Method:

X-RAY DIFFRACTION

Resolution:

2.13 Å

R-Value Free:

0.21

R-Value Work:

0.21

R-Value Observed:

0.21

Space Group:

I 2 3

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Macromolecular Entities

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:Epidermal growth factor recep
Gene (Uniprot):EGFR
Chain IDs:A
Chain Length:327
Number of Molecules:1
Biological Source:Homo sapiens

UniProt ID:P00533 Pfam ID:PF07714 EC:2.7.10.1

Ligand Molecules

A1A6K

MES

Primary Citation

Structural Studies of Fourth-Generation EGFR Inhibitors Reveal Insights into Selective T790M and C797S Targeting.

Damghani, T, Song, S, Lin, K.S, Li, J, Heppner, D.E.Show

Acs Med.Chem.Lett. ? ? ? (2026)

PMID: 41684669 DOI: 10.1021/acsmedchemlett.5c00725

Abstact

Inhibitors targeting mutant EGFR remain a persistent need in combating drug resistance in non-small cell lung cancer. To better understand the molecular factors involved in targeting T790M and C797S mutations, we determined X-ray cocrystal structures of fourth-generation inhibitors BI-8128 and BI-4732. Analysis from molecular dynamics and thermodynamic integration calculations correlated with biochemical and cellular measurements indicate that BI-8128 binds the double T790M/C797S more strongly than the single mutations individually. This observation showcases strengths in the design of these fourth-generation EGFR inhibitors as profile criteria require drugs to inhibit an array of oncogenic and drug resistance mutations.

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Protein

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Disease

Primary Citation of related structures

Abstact

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