9IGD image
Deposition Date 2025-02-19
Release Date 2026-06-24
Last Version Date 2026-06-24
Entry Detail
PDB ID:
9IGD
Keywords:
APOPTOSIS
Title:
Structure of human Bcl-xL in complex with small molecule inhibitor
Biological Source:
Source Organism(s):
Homo sapiens (Taxon ID: 9606)
Expression System(s):
Escherichia coli bl21
Method Details:
Experimental Method:
X-RAY DIFFRACTION
Resolution:
2.40 Å
R-Value Free:
0.22
R-Value Work:
0.18
R-Value Observed:
0.18
Space Group:
P 43 21 2
9IGD validation report missing
Macromolecular Entities
Protein Blast
Polymer Type:polypeptide(L)
Molecule:Apoptosis regulator Bcl-2,Bcl
Gene (Uniprot):BCL2, BCL2L1
Chain IDs:A, B
Chain Length:159
Number of Molecules:2
Biological Source:Homo sapiens
UniProt ID:P10415,Q07817 Pfam ID:PF02180, PF00452
Ligand Molecules
A1I37
CL
Primary Citation
Structure-Based Discovery of Potent BCL-XL Inhibitors through Rescaffolding.
J.Med.Chem. ? ? ? (2026)
PMID: 42283755 DOI: 10.1021/acs.jmedchem.6c00865

Abstact

Evasion of apoptosis is a hallmark of cancer. Deregulation of BCL-XL, a member of the BCL-2 family of proteins, has been linked to the development of various tumor types. This study presents the design and synthesis of BCL-XL inhibitors with novel mono- and bicyclic cores. The new structural features were optimized to combine high binding efficiency with the opening of diverse novel vectors for additional modifications. The lead compounds exhibited picomolar affinities and significant cellular potency in the BCL-XL-dependent MOLT-4 cell line, which also translated into marked tumor growth inhibition in a xenograft study. These findings highlight the potential of BCL-XL inhibitors as therapeutic agents in cancer treatment by targeting the apoptotic intrinsic pathway.

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Primary Citation of related structures
9I9E
9IGB
9IGC
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