Target specificity of selective bioactive compounds in blocking α-dystroglycan receptor to suppress Lassa virus infection: an &lt;i&gt;in&lt;/i&gt; &lt;i&gt;silico&lt;/i&gt; approach

Arefin, Adittya; Ema, Tanzila Ismail; Islam, Tamnia; Hossen, Saddam; Islam, Tariqul; Azad, Salauddin Al; Badal, Nasir Uddin; Islam, Aminul; Biswas, Partha; Alam, Nafee Ul; Islam, Enayetul; Anjum, Maliha; Masud, Afsana; Kamran, Shaikh; Rahman, Ahsab; Paul, Parag Kumar

doi:10.7555/jbr.35.20210111

Cited by 41 publications

(30 citation statements)

References 54 publications

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“…In the quantitative observation, eight binding pockets were estimated for the hACE2 receptor protein, obtained from the COACH-D algorithm [ 22 , 23 ]. After evaluating the predicted binding energy and involvement of particular residues, the top binding pockets were chosen from the eight found ( Fig.…”

Section: Methodsmentioning

confidence: 99%

“…The pharmacokinetic properties of isovitexin following its absorption, distribution, metabolism, elimination, and toxicity (ADMET) and quantitative structure–activity relationship (QSAR) profiles were studied [ 24 ]. The parameters that followed Lipinski’s rule were initially evaluated using Swiss ADME and Molinspiration Cheminformatics [ 22 ]. Finally, the toxicity level was analyzed using the pkCSM server system [ 23 ].…”

Section: Methodsmentioning

confidence: 99%

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Point-specific interactions of isovitexin with the neighboring amino acid residues of the hACE2 receptor as a targeted therapeutic agent in suppressing the SARS-CoV-2 influx mechanism

et al. 2022

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Objective: Despite the development of several vaccines against severe acute respiratory syndrome coronavirus-2, the need for an additional prophylactic agent is evident. In recent in silico studies, isovitexin exhibited a higher binding affinity against the human angiotensin converting-enzyme 2 (hACE2) receptor than existing antiviral drugs. The research aimed to find out the point specificity of isovitexin for the hACE2 receptor and to assess its therapeutic potential, depending on the stability of the isovitexin–hACE2 complex. Materials and Methods: The pharmacokinetic profile of isovitexin was analyzed. The crystal structure of the hACE2 receptor and the ligand isovitexin were docked to form a ligand-protein complex following molecular optimization. To determine the isovitexin–hACE2 complex stability, their binding affinity, hydrogen bonding, and hydrophobic interactions were studied. Lastly, the root mean square deviation (RMSD), root mean square fluctuation, solvent accessible surface area, molecular surface area, radius of gyration (Rg), polar surface area, and principal component analysis values were found by simulating the complex with molecular dynamic (MD). Results: The predicted Lethal dose50 for isovitexin was 2.56 mol/kg, with an acceptable maximum tolerated dose and no hepatotoxicity or AMES toxicity. Interactions with the amino acid residues Thr371, Asp367, Glu406, Pro346, His345, Phe274, Tyr515, Glu375, Thr347, Glu402, and His374 of the hACE2 protein were required for the high binding affinity and specificity of isovitexin. Based on what was learned from the MD simulation, the hACE2 receptor-blocking properties of isovi¬texin were looked at. Conclusions: Isovitexin is a phytochemical with a reasonable bioactivity and safety profile for use in humans, and it can potentially be used as a hACE2-specific therapeutic to inhibit COVID-19 infection.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Point-specific interactions of isovitexin with the neighboring amino acid residues of the hACE2 receptor as a targeted therapeutic agent in suppressing the SARS-CoV-2 influx mechanism

et al. 2022

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“…A high resolution (2.4 Å) 3D crystal structure of TLR2 (PDB ID: 3A7C) was selected from the protein data bank (Berman et al 2003) and converted to PDB format. This structure was then processed to present the proper size, orientation, and rotations of the protein (Arefin et al 2021). The processing was carried out in UCSF Chimera (version 1.14) (https://www.cgl.ucsf.edu/chimera/) to remove non-standard amino acids, water molecules, ligands and ions, add missing hydrogen atoms, and to perform energy minimization of the protein structure (Yang et al 2012).…”

Section: Methodsmentioning

confidence: 99%

Metformin, empagliflozin and their combination modulate ex-vivo macrophage inflammatory gene expression

Arefin

Gage

2022

Preprint

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Type-2 Diabetes Mellitus is a complex, chronic illness characterized by persistent high blood glucose levels. Patients can be prescribed anti-diabetes drugs as single agents or in combination depending on the severity of their condition. Metformin and empagliflozin are two commonly prescribed anti-diabetes drugs which reduce hyperglycemia, however their direct effects on macrophage inflammatory responses alone or in combination are unreported. Here we show that metformin and empagliflozin elicit proinflammatory responses on mouse bone-marrow derived macrophages with single agent challenge, which are modulated when added in combination. In-silico docking experiments suggested that empagliflozin can interact with both TLR2 and DECTIN1 receptors and we observed that both empagliflozin and metformin increase expression of Tlr2 and Clec7a. Thus, findings from this study suggest that metformin and empagliflozin as single agents or in combination can directly modulate inflammatory gene expression in macrophages and upregulate the expression of their receptors.

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“…Salvicine-induced DNA DSBs activate ATM and ATR kinases, as well as histone H2AX phosphorylation, in A549 lung cancer cells, which has been widely described in DSB-induced cellular responses ( 149 , 150 ). Salvicine inhibits the catalytic subunit of DNA-dependent protein kinase (DNA-PK), but not the Ku70 or Ku86 subunits, which is surprising.…”

Section: Ros-induced and Topo Ii-dependent Dna Damage Response And Ap...mentioning

confidence: 99%

Investigating the Anticancer Potential of Salvicine as a Modulator of Topoisomerase II and ROS Signaling Cascade

Dey

Hasan

Biswas³

et al. 2022

Front. Oncol.

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Salvicine is a new diterpenoid quinone substance from a natural source, specifically in a Chinese herb. It has powerful growth-controlling abilities against a broad range of human cancer cells in both in vitro and in vivo environments. A significant inhibitory effect of salvicine on multidrug-resistant (MDR) cells has also been discovered. Several research studies have examined the activities of salvicine on topoisomerase II (Topo II) by inducing reactive oxygen species (ROS) signaling. As opposed to the well-known Topo II toxin etoposide, salvicine mostly decreases the catalytic activity with a negligible DNA breakage effect, as revealed by several enzymatic experiments. Interestingly, salvicine dramatically reduces lung metastatic formation in the MDA-MB-435 orthotopic lung cancer cell line. Recent investigations have established that salvicine is a new non-intercalative Topo II toxin by interacting with the ATPase domains, increasing DNA–Topo II interaction, and suppressing DNA relegation and ATP hydrolysis. In addition, investigations have revealed that salvicine-induced ROS play a critical role in the anticancer-mediated signaling pathway, involving Topo II suppression, DNA damage, overcoming multidrug resistance, and tumor cell adhesion suppression, among other things. In the current study, we demonstrate the role of salvicine in regulating the ROS signaling pathway and the DNA damage response (DDR) in suppressing the progression of cancer cells. We depict the mechanism of action of salvicine in suppressing the DNA–Topo II complex through ROS induction along with a brief discussion of the anticancer perspective of salvicine.

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Target specificity of selective bioactive compounds in blocking α-dystroglycan receptor to suppress Lassa virus infection: an <i>in</i> <i>silico</i> approach

Cited by 41 publications

References 54 publications

Point-specific interactions of isovitexin with the neighboring amino acid residues of the hACE2 receptor as a targeted therapeutic agent in suppressing the SARS-CoV-2 influx mechanism

Point-specific interactions of isovitexin with the neighboring amino acid residues of the hACE2 receptor as a targeted therapeutic agent in suppressing the SARS-CoV-2 influx mechanism

Metformin, empagliflozin and their combination modulate ex-vivo macrophage inflammatory gene expression

Investigating the Anticancer Potential of Salvicine as a Modulator of Topoisomerase II and ROS Signaling Cascade

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