MicroRNA 132-3p Is Upregulated in Laron Syndrome Patients and Controls Longevity Gene Expression

The growth hormone (GH)–insulin-like growth factor-1 (IGF1) endocrine axis is a central player in normal growth and metabolism as well as in a number of pathologies, including cancer. The GH–IGF1 hormonal system, in addition, has emerged as a major determinant of lifespan and healthspan. Laron syndrome (LS), the best characterized entity under the spectrum of the congenital IGF1 deficiencies, results from mutation of the GH receptor (GHR) gene, leading to dwarfism, obesity and other defects. Consistent with the key role of IGF1 in cellular proliferation, epidemiological studies have shown that LS patients are protected from cancer development. While reduced expression of components of the GH-IGF1 axis is associated with enhanced longevity in animal models, it is still unknown whether LS is associated with an increased lifespan. MicroRNAs (miRs) are endogenous short non-coding RNAs that regulate the expression of complementary mRNAs. While a number of miRs involved in the regulation of IGF components have been identified, no previous studies have investigated the differential expression of miRs in congenital IGF1 deficiencies. The present study was aimed at identifying miRs that are differentially expressed in LS and that might account for the phenotypic features of LS patients, including longevity. Our genomic analyses provide evidence that miR-132-3p was highly expressed in LS. In addition, we identified SIRT1, a member of the sirtuin family of histone deacetylases, as a target for negative regulation by miR-132-3p. The data was consistent with the notion that low concentrations of IGF1 in LS lead to elevated miR-132-3p levels, with ensuing reduction in SIRT1 gene expression. The impact of the IGF1-miR-132-3p-SIRT1 loop on aging merits further investigation.     

Adsorption of volatile aroma compound 2-phenylethanol from synthetic solution onto granular activated carbon in batch and continuous modes

This paper reports a study on the adsorption of the aroma component 2-phenylethanol from an aqueous solution onto granular activated carbon, derived from coconut husks, using batch and continuous (packed-bed column) systems. In the batch mode, the contact time required to attain the adsorption equilibrium was 90 min. The adsorption isotherms were evaluated at 20.0 °C, 30.0 °C and 40.0 °C. In the continuous mode, the effects of flow rate and bed length were studied. Experimental data showed that the breakthrough and exhaustion times decreased with higher flow rates and increased with higher packed beds. The adsorption in the fixed-bed column was more efficient under the following conditions: flow rate of 3.5 mL min⁻¹ and bed length of 11 cm. Based on the data acquired, adsorption appears to represent a promising method for the recovery of 2-phenylethanol lost during the instant coffee production process.     

MPI8 is Potent against SARS-CoV-2 by Inhibiting Dually and Selectively the SARS-CoV-2 Main Protease and the Host Cathepsin L**

A number of inhibitors have been developed for the SARS-CoV-2 main protease (M^Pro) as potential COVID-19 medications but little is known about their selectivity. Using enzymatic assays, we characterized inhibition of TMPRSS2, furin, and cathepsins B/K/L by more than a dozen of previously developed M^Pro inhibitors including MPI1-9, GC376, 11a, 10–1, 10–2, and 10–3. MPI1-9, GC376 and 11a all contain an aldehyde for the formation of a reversible covalent hemiacetal adduct with the M^Pro active site cysteine and 10–1, 10–2 and 10–3 contain a labile ester to exchange with the M^Pro active site cysteine for the formation of a thioester. Our data revealed that all these inhibitors are inert toward TMPRSS2 and furin. Diaryl esters also showed low inhibition of cathepsins. However, all aldehyde inhibitors displayed high potency in inhibiting three cathepsins. Their determined IC₅₀ values vary from 4.1 to 380 nM for cathepsin B, 0.079 to 2.3 nM for cathepsin L, and 0.35 to 180 nM for cathepsin K. All aldehyde inhibitors showed similar inhibition levels toward cathepsin L. A cellular analysis indicated high potency of MPI5 and MPI8 in inhibiting lysosomal activity, which is probably attributed to their inhibition of cathepsins. Among all aldehyde inhibitors, MPI8 shows the best selectivity toward cathepsin L. With respect to cathepsins B and K, the selective indices are 192 and 150, respectively. MPI8 is the most potent compound among all aldehyde inhibitors in cellular M^Pro inhibition potency and anti-SARS-CoV-2 activity in Vero E6 cells. Cathepsin L has been demonstrated to play a critical role in the SARS-CoV-2 cell entry. By selectively inhibiting both SARS-CoV-2 M^Pro and the host cathepsin L, MPI8 potentiates dual inhibition effects to synergize its overall antiviral potency and efficacy. Due to its high selectivity toward cathepsin L that reduces potential toxicity toward host cells and high cellular and antiviral potency, we urge serious consideration of MPI8 for preclinical and clinical investigations for treating COVID-19.     

Chemical Tools to Study Bacterial Glycans: A Tale from Discovery of Glycoproteins to Disruption of Their Function

Bacteria coat themselves with a dense array of cell envelope glycans that enhance bacterial fitness and promote survival. Despite the importance of bacterial glycans, their systematic study and perturbation remains challenging. Chemical tools have made important inroads toward understanding and altering bacterial glycans. This review describes how pioneering discoveries from Prof. Carolyn Bertozzi's laboratory inspired our laboratory to develop sugar probes to facilitate the study of bacterial glycans. As described below, we used metabolic glycan labelling to install bioorthogonal reporters into bacterial glycans, ultimately permitting the discovery of a protein glycosylation system, the identification of glycosylation genes, and the development of metabolic glycan inhibitors. Our results have provided an approach to screen bacterial glycans and gain insight into their function, even in the absence of detailed structural information.     

Reticulated open-cellular aluminum nitride ceramic foams: Effect of sintering aids on microstructural,thermal, and mechanical properties

Open-celled aluminum nitride ceramic foams were prepared by the polymer sponge replication technique involving aqueous dispersions of passivated AlN. The amount of the Y₂O₃ and Dy₂O₃ as sintering aid was varied, and the effects on the densification, microstructure formation, phase composition, and finally, the thermal conductivity were investigated. A typical thermal conductivity of 1.1 W m⁻¹ K⁻¹ was determined for foams at a porosity level of 94.3 vol.%, on average. This measured foam thermal conductivity was subsequently modeled using different porosity ↔ thermal conductivity relations considering the different hierarchical levels of porosity in these foams. From these models, the thermal conductivity of the bulk AlN strut material was determined, correlated with the strut microstructure and the phase composition, and compared to literature data.