3.A.1.5.42
Peptide transporter, SapABCDF. The Sap transport system renders resistance against host-produced
antimicrobial peptides (AMPs) amongst various Gram-negative bacteria (Dasgupta and Kanaujia 2025).
The Sap system imports the AMPs across the membrane into the cytoplasm,
wherein they are cleaved by proteases. The membrane components (SapBCDF) may also function as a putrescine
exporter. Its
multifaceted attributes in the uptake of dipeptides, AMPs, and heme were examined using molecular dynamics
simulations of EcSapA in its apo and holo (bound to dipeptides, AMPs,
and heme) forms. Ths was performed to gain structural insights into its
molecular plasticity. The results suggest that EcSapA
possesses a wide and promiscuous binding site that is favorable for
accommodating varying lengths of ligands with a ligand-dependent
conformational dynamics mechanism. The estimated binding
energies of the ligands suggest that EcSapA shows a preferential binding
for cationic AMPs, followed by heme and dipeptides (Dasgupta and Kanaujia 2025).
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| Accession Number: | P0AAH4 |
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| Protein Name: | Peptide transport system ATP-binding protein SapD |
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| Length: | 330 |
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| Molecular Weight: | 37661.00 |
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| Species: | Escherichia coli (strain K12) [83333] |
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| Location1 / Topology2 / Orientation3: |
Cell inner membrane1 / Peripheral membrane protein2 |
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| Substrate |
peptide |
|---|
1: MPLLDIRNLT IEFKTGDEWV KAVDRVSMTL TEGEIRGLVG ESGSGKSLIA KAICGVNKDN
61: WRVTADRMRF DDIDLLRLSA RERRKLVGHN VSMIFQEPQS CLDPSERVGR QLMQNIPAWT
121: YKGRWWQRFG WRKRRAIELL HRVGIKDHKD AMRSFPYELT EGECQKVMIA IALANQPRLL
181: IADEPTNSME PTTQAQIFRL LTRLNQNSNT TILLISHDLQ MLSQWADKIN VLYCGQTVET
241: APSKELVTMP HHPYTQALIR AIPDFGSAMP HKSRLNTLPG AIPLLEQLPI GCRLGPRCPY
301: AQRECIVTPR LTGAKNHLYA CHFPLNMEKE