Structural insights into substrate and inhibitor binding sites in human indoleamine 2,3-dioxygenase 1

Lewis-Ballester, Ariel; Pham, Khoa; Batabyal, Dipanwita; Karkashon, Shay; Bonanno, J.B.; Poulos, T.L.; Yeh, Syun Ru

doi:10.1038/s41467-017-01725-8

Cited by 136 publications

(265 citation statements)

References 42 publications

(46 reference statements)

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“…Results have allowed disclosing for the first time high and low dissociation constants (K d ) of l ‐Trp to IDO1, as well as the presence of a metastable interaction site located close to the C‐terminal part of the JK‐loop and defined by Lys238. Furthermore, results provide an additional support to the reported key role of the C‐terminal part of the JK‐loop in regulating the catalytic activity of the enzyme …”

Section: Introductionsupporting

confidence: 74%

“…Of note, the importance of such loop in controlling the catalytic activity of IDO1 was independently reported in literature by distinct research groups . In particular, other studies used different molecular dynamic approaches in combination with mutagenesis experiments (Thr379Ala) to show that the conserved “GTGG” motif of JK‐loop C affects the binding of substrate to IDO1, adopting closed and open conformational states .…”

Section: Resultsmentioning

confidence: 99%

“…According to crystallographic studies, the inhibitory substrate pocket is located below the plane of the heme group and defined by residues Phe270, Asp274 and Arg343 . The authors generated the Phe270Gly IDO1 mutant for increasing the plasticity of the site and thus allowing the capture of one molecule of l ‐Trp into the inhibitory substrate pocket.…”

Section: Resultsmentioning

confidence: 99%

“…Only productive steps were saved to generate suMD trajectories that were then analyzed. RMSD values (Å) of ligand along trajectories of models A–C were calculated from the atomic coordinates of l ‐Trp heavy atoms as obtained in the substrate co‐crystal structure of IDO1 (pdb code: 5WMU) . Ligand‐protein interaction energy was calculated using NAMD Energy extension available in VMD .…”

Section: Methodsmentioning

confidence: 99%

“…Moreover, disappointing results have been very recently reported for the most advanced IDO1 inhibitor, i. e. epacadostat ( 4 ), and compound 6 and 7 have also been withdrawn from the clinic . Additional studies have sought to better understand the complex biology of the enzyme and aid the design and development of next‐generation IDO1 inhibitors . In the current report, we investigated the molecular recognition path of l ‐Trp ( 1 ) to human IDO1 through a synergic approach based on microscale thermophoresis, supervised molecular dynamics (SuMD) and mutagenesis experiments.…”

Section: Introductionmentioning

confidence: 99%

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Tracking Hidden Binding Pockets Along the Molecular Recognition Path of l‐Trp to Indoleamine 2,3‐Dioxygenase 1

et al. 2019

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Indoleamine 2,3-dioxygenase 1 (IDO1) catalyzes the oxidative cleavage of l-Tryptophan (l-Trp) to yield N-formyl-kynurenine in the first and rate limiting step of the kynurenine pathway. Bioactive metabolites, involved in the regulation of important immunological responses and neurological processes, are then produced by downstream enzymes along the pathway. Inhibitors of IDO1 are being designed and developed as therapeutic agents for immuno-oncology. In this work, we investigated the molecular recognition path of l-Trp to IDO1, integrating biophysical methods with supervised molecular dynamics (suMD) and mutagenesis experiments. Results allowed disclosing for the first time high and low dissociation constants of l-Trp to IDO1, and the presence of a metastable interaction site located at the upper part of a channel whose borders are defined by the EF-loop and the C-terminal part of the JK-loop. Collectively, our results provide new clues for the design of next-generation IDO1 ligands.[a] Dr. interaction energy was calculated using NAMD Energy extension available in VMD. [55] The latter was used to render images and prepare movies of trajectories (ModelA.mpg, ModelB.mpg, Mod-elC.mpg; supporting information). 4 5 6 7 8

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Section: Introductionsupporting

confidence: 74%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Tracking Hidden Binding Pockets Along the Molecular Recognition Path of l‐Trp to Indoleamine 2,3‐Dioxygenase 1

et al. 2019

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Tumor Cell‐Responsive Photodynamic Immunoagent for Immunogenicity‐Enhanced Orthotopic and Remote Tumor Therapy

Chen

Xiong

Zhao

et al. 2022

Adv Healthcare Materials

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Combining photodynamic therapy (PDT) and immune checkpoint blockades is an efficient method to maximize immunotherapeutic outcome by boosting tumor immunogenicity and modulating the immunosuppressive tumor microenvironment. However, the always‐on bioactivity of photosensitizers or immune checkpoint inhibitors leads to uncontrollable side effects, limiting the in vivo therapeutic efficacy of treatments. An activatable strategy is of great importance for improving the selectivity during cancer therapy. In this study, a photodynamic immunomodulator, ICy‐NLG, is developed by conjugating the photosensitizer ICy‐NH2 with the indoleamine 2,3‐dioxygenase 1 inhibitor NLG919 through a glutathione (GSH)‐cleavable linker to achieve activatable photodynamic immunotherapy. The conjugation considerably suppresses both the PDT effect and the activity of the inhibitor. After ICy‐NLG is activated by high levels of GSH in tumor cells, the PDT effect is restored and leads to immunogenic tumor cell death. The released tumor‐associated antigens in conjunction with the activated immune checkpoint inhibitor induce a synergistic antitumor immune response, resulting in the growth inhibition of primary and distant tumors and the prevention of lung metastasis in mouse xenograft models.

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Dual‐Responsive Supramolecular Polymeric Nanomedicine for Self‐Cascade Amplified Cancer Immunotherapy

Hu,

Ye,

et al. 2024

Advanced Science

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Insufficient tumor immunogenicity and immune escape from tumors remain common problems in all tumor immunotherapies. Recent studies have shown that pyroptosis, a form of programmed cell death that is accompanied by immune checkpoint inhibitors, can induce effective immunogenic cell death and long‐term immune activation. Therapeutic strategies to jointly induce pyroptosis and reverse immunosuppressive tumor microenvironments are promising for cancer immunotherapy. In this regard, a dual‐responsive supramolecular polymeric nanomedicine (NCSNPs) to self‐cascade amplify the benefits of cancer immunotherapy is designed. The NCSNPs are formulated by β‐cyclodextrin coupling nitric oxide (NO) donor, a pyroptosis activator, and NLG919, an indoleamine 2,3‐dioxygenase (IDO) inhibitor, and self‐assembled through host–guest molecular recognition and hydrophobic interaction to obtain nanoparticles. NCSNPs possess excellent tumor accumulation and bioavailability attributed to ingenious supramolecular engineering. The study not only confirms the occurrence of NO‐triggered pyroptosis in tumors for the first time but also reverses the immunosuppressive microenvironment in tumor sites via an IDO inhibitor by enhancing the infiltration of cytotoxic T lymphocytes, to achieve remarkable inhibition of tumor proliferation. Thus, this study provides a novel strategy for cancer immunotherapy.

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Structural insights into substrate and inhibitor binding sites in human indoleamine 2,3-dioxygenase 1

Cited by 136 publications

References 42 publications

Tracking Hidden Binding Pockets Along the Molecular Recognition Path of l‐Trp to Indoleamine 2,3‐Dioxygenase 1

Tracking Hidden Binding Pockets Along the Molecular Recognition Path of l‐Trp to Indoleamine 2,3‐Dioxygenase 1

Tumor Cell‐Responsive Photodynamic Immunoagent for Immunogenicity‐Enhanced Orthotopic and Remote Tumor Therapy

Dual‐Responsive Supramolecular Polymeric Nanomedicine for Self‐Cascade Amplified Cancer Immunotherapy

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