Arylamide as Potential Selective Inhibitor for Matrix Metalloproteinase 9 (MMP9): Design, Synthesis, Biological Evaluation, and Molecular Modeling

Hariono, Maywan; Nuwarda, Rina Fajri; Yusuf, Muhammad; Rollando, Rollando; Jenie, Riris Istighfari; Al-Najjar, Belal O.; Julianus, Jeffry; Putra, Kevin Cahaya; Nugroho, Ervan S.; Wisnumurti, Yohanes Krisna; Dewa, Sangga Putra; Jati, Benedictus Wisnu Putra; Tiara, Reynaldo; Ramadani, Ratna Dwi; Qodria, Lailatul; Wahab, Habibah A.

doi:10.1021/acs.jcim.9b00630

Cited by 19 publications

(18 citation statements)

References 53 publications

(102 reference statements)

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“…To determine the cytotoxicity of each extract on 4T1, T47D, and Vero cells, the MTT assay was employed. 4T1 is a triple-negative breast cancer cell line from Mus musculus [ 54 ] that contains PEX9 showing 61% homology with PDB 1ITV upon Blast Analysis [ 55 ]. T47D is a cell model to characterize the progesterone-specific effect of a luminal A subtype of breast cancer [ 56 ], whereas Vero cell is a non-tumorigenic cell from the kidney tissue of African green monkey [ 57 ].…”

Section: Methodsmentioning

confidence: 99%

Bioguided Fractionation of Local Plants against Matrix Metalloproteinase9 and Its Cytotoxicity against Breast Cancer Cell Models: In Silico and In Vitro Study

et al. 2020

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Matrix metalloproteinase9 (MMP9) is known to be highly expressed during metastatic cancer where most known potential inhibitors failed in the clinical trials. This study aims to select local plants in our state, as anti-breast cancer agent with hemopexin-like domain of MMP9 (PEX9) as the selective protein target. In silico screening for PEX9 inhibitors was performed from our in house-natural compound database to identify the plants. The selected plants were extracted using methanol and then a step-by-step in vitro screening against MMP9 was performed from its crude extract, partitions until fractions using FRET-based assay. The partitions were obtained by performing liquid–liquid extraction on the methanol extract using n-hexane, ethylacetate, n-butanol, and water representing nonpolar to polar solvents. The fractions were made from the selected partition, which demonstrated the best inhibition percentage toward MMP9, using column chromatography. Of the 200 compounds screened, 20 compounds that scored the binding affinity −11.2 to −8.1 kcal/mol toward PEX9 were selected as top hits. The binding of these hits were thoroughly investigated and linked to the plants which they were reported to be isolated from. Six of the eight crude extracts demonstrated inhibition toward MMP9 with the IC50 24 to 823 µg/mL. The partitions (1 mg/mL) of Ageratum conyzoides aerial parts and Ixora coccinea leaves showed inhibition 94% and 96%, whereas their fractions showed IC50 43 and 116 µg/mL, respectively toward MMP9. Using MTT assay, the crude extract of Ageratum exhibited IC50 22 and 229 µg/mL against 4T1 and T47D cell proliferations, respectively with a high safety index concluding its potential anti-breast cancer from herbal.

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Section: Methodsmentioning

confidence: 99%

Bioguided Fractionation of Local Plants against Matrix Metalloproteinase9 and Its Cytotoxicity against Breast Cancer Cell Models: In Silico and In Vitro Study

et al. 2020

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“…Peptides generated to mimic the outer beta strand of blade I or IV resulted in decreased levels of MMP9 dimers and also a reduction cell migration [33]. MMP-9 can also increase angiogenesis [38]. Using an allosteric inhibitor to the PEX domain, Hariono et al [38] demonstrated that inhibition of ECM proteolysis, which decreases release of vascular endothelial growth factor (VEGF) from within the ECM, significantly reduces binding of VEGF to its membrane receptor and subsequently, decreases angiogenesis.…”

Section: Non-proteolytic Functions Of Mmpsmentioning

confidence: 99%

“…MMP-9 can also increase angiogenesis [38]. Using an allosteric inhibitor to the PEX domain, Hariono et al [38] demonstrated that inhibition of ECM proteolysis, which decreases release of vascular endothelial growth factor (VEGF) from within the ECM, significantly reduces binding of VEGF to its membrane receptor and subsequently, decreases angiogenesis. broad-spectrum compounds [42].…”

Section: Non-proteolytic Functions Of Mmpsmentioning

confidence: 99%

“…Strategies to inhibit MMP functions with small molecules has been explored ( Table 2) [ 33,38,40,41,45]. In silico analysis of MMP9 in which molecular docking programs were utilized to map potential ligand binding sites in the PEX domain at the dimerization interface were successful at identifying compound that interfered with MMP9 homodimerization and blocked a downstream signaling pathway critical for MMP9 mediated cell migration and invasion [46].…”

Section: Small Molecule Mmp Inhibitorsmentioning

confidence: 99%

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The Pharmacological Tails of Matrix Metalloproteinases and Their Inhibitors

Das¹,

Benko²,

Gill³

et al. 2020

Preprint

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Matrix metalloproteinases (MMPs) have been demonstrated to have both detrimental and protective functions in inflammatory diseases. Several MMP inhibitors, with the exception of Periostat®, have failed in Phase III clinical trials. As an alternative strategy, recent efforts have been focussed on the development of more selective inhibitors or targeting other domains than their active sites (e.g., exosites, ectosites) through specific small molecule inhibitors or monoclonal antibodies. Here, we present some examples that aim to better understand the mechanisms of conformational changes/allosteric control of MMPs functions. In addition to MMP inhibitors, we discuss unbiased global approaches such as proteomics and N-terminomics to identify new MMP substrates and achieve a better understanding of the roles of these proteases in diseases.

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“…Other attempts have been made to target exosite domains, such as the HPX domain, which are less conserved. Several exosite inhibitors abrogated cancer cell migration through specific prevention of the association of pro-MMP-9 with both α4β1 integrin and CD44 without modulating the catalytic activity of MMP-9 [21][22][23]. Although exosite recognition could contribute to improving the specificity of active-site inhibitors, it remains difficult to obtain specific active-site inhibitors against a single MMP.…”

Section: Introductionmentioning

confidence: 99%

Discovery of potent and specific inhibitors targeting the active site of MMP-9 from the engineered SPINK2 library

et al. 2020

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Matrix metalloproteinases (MMPs) contribute to many physiological and pathological phenomena via the proteolysis of extracellular matrix components. Specific blocking of the active site of each MMP sheds light on its particular role. However, it remains difficult to acquire an active-site inhibitor with high specificity for only the target MMP due to the highly conserved structure around the active site of MMPs. Recently, we reported that potent and specific inhibitors of serine proteases were obtained from our proprietary engineered serine protease inhibitor Kazal type 2 (SPINK2) library. In this research, using this library, we succeeded in obtaining potent and specific MMP-9 inhibitors. The obtained inhibitors bound to the active site of MMP-9 and inhibited MMP-9 with low nanomolar Ki values. The inhibitors did not cross-react with other MMPs that we tested. Further analysis using MMP-9 mutants demonstrated that the inhibitors recognize not only the residues around the conserved active site of MMP-9 but also different and unique residues in exosites that are distant from each other. This unique recognition manner, which can be achieved by the large interface provided by engineered SPINK2, may contribute to the generation of specific active-site inhibitors of MMPs.

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Arylamide as Potential Selective Inhibitor for Matrix Metalloproteinase 9 (MMP9): Design, Synthesis, Biological Evaluation, and Molecular Modeling

Cited by 19 publications

References 53 publications

Bioguided Fractionation of Local Plants against Matrix Metalloproteinase9 and Its Cytotoxicity against Breast Cancer Cell Models: In Silico and In Vitro Study

Bioguided Fractionation of Local Plants against Matrix Metalloproteinase9 and Its Cytotoxicity against Breast Cancer Cell Models: In Silico and In Vitro Study

The Pharmacological Tails of Matrix Metalloproteinases and Their Inhibitors

Discovery of potent and specific inhibitors targeting the active site of MMP-9 from the engineered SPINK2 library

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