Lorenzo Giordano scite author profile

Lorenzo Giordano

3Publications

32Citation Statements Received

99Citation Statements Given

How they've been cited

How they cite others

175

Affiliations

University of Rome Tor Vergata

Publications

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The Lipid Dependence of Antimicrobial Peptide Activity Is an Unreliable Experimental Test for Different Pore Models

et al. 2012

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The role played by glutathione transferase P1-1 (GSTP1-1) in modulating the c-Jun N-terminal kinase (JNK) pathway has been extensively investigated using JNK isoforms known to exert opposite effects in the cells. We have expressed isoform JNK1α2, which has been reported to transmit a pro-apoptotic signal, and we have analyzed both the phosphorylation level and the activity of this kinase in the presence of GSTP1-1. Contrary to what previous studies suggest, we found that GSTP1-1 is able to form a complex with the unphosphorylated and inactive JNK1α2 isoform, even in the absence of the substrate. We also analyzed the consequences of this interaction on the activity of both enzymes. The complex strongly reduced the extent of activation of JNK1α2 and preserved GSTP1-1 from inactivation. Unexpectedly, glutathione (GSH) exerted a negative effect on the affinity of GSTP1-1 for JNK1α2, suggesting that the intracellular levels of this thiol may allow a fine-tuning of the MAPK signaling pathway. Moreover, we found that the adduct formed by GSH and the strong GSTP1-1 inhibitor NBDHEX abolishes the interaction between GSTP1-1 and JNK1α2. These data confirm and extend at the molecular level previous evidence obtained in tumor cell lines.

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Effects of antimicrobial peptides on membrane dynamics: A comparison of fluorescence and NMR experiments

Roversi

Troiano

Salnikov

et al. 2023

Biophysical Chemistry

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Membrane Perturbing Effects of Antimicrobial Peptides: A Systematic Spectroscopic Analysis

Roversi

Giordano

Zotti

et al. 2013

Biophysical Journal

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to PG-containing bilayers, which has been described by the electrostatic attraction and surface partitioning model. [2] FRET experiments supported the clustering of GM1, but not PG, by MG2. Quenching data suggested that MG2 is bound to the sugar region of GM1. The bound peptide assumed a helical structure and induced the leakage of calcein and the coupled flip-flop of lipids, indicating the peptide also forms a toroidal pore in GM1-containing vesicles. However, the membrane permeabilization activity against GM1-containing membranes was weaker than that against PG-doped liposomes in accordance with the trapping of the peptide in the sugar region. These data shed light on AMP-human cell interaction. References. [1] Matsuzaki K (2009) Control of cell selectivity of antimicrobial peptides.

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