Maria Luisa Mangoni | Ricerc@Sapienza

Pubblicazioni

Titolo	Pubblicato in	Anno
Cell-density dependence of host-defense peptide activity and selectivity in the presence of host cells	ACS CHEMICAL BIOLOGY	2017
Effects of aib residues insertion on the structural–functional properties of the frog skin-derived peptide esculentin-1a(1–21)NH2	AMINO ACIDS	2017
Methods for in vivo/ex vivo analysis of antimicrobial peptides in bacterial keratitis: SiRNA knockdown, colony counts, myeloperoxidase, immunostaining, and RT-PCR assays	Methods in Molecular Biology	2017
Promising approaches to optimize the biological properties of the antimicrobial peptide esculentin-1a(1-21)NH2. amino acids substitution and conjugation to nanoparticles	FRONTIERS IN CHEMISTRY	2017
Cytotoxic peptides with insulin-releasing activities from skin secretions of the Italian stream frog Rana italica (Ranidae)	JOURNAL OF PEPTIDE SCIENCE	2017
In vivo therapeutic efficacy of frog skin-derived peptides against Pseudomonas aeruginosa-induced pulmonary infection	SCIENTIFIC REPORTS	2017
Membrane perturbing activities and structural properties of the frog-skin derived peptide esculentin-1a(1-21)NH2 and its diastereomer esc(1-21)-1c: correlation with their antipseudomonal and cytotoxic activity	BIOCHIMICA ET BIOPHYSICA ACTA-BIOMEMBRANES	2017
Characterization of anti-biofilm peptide activity: a biophysical approach	BIOPHYSICAL JOURNAL	2017
Glycine-replaced derivatives of [Pro3,DLeu9]TL, a temporin L analogue: evaluation of antimicrobial, cytotoxic and hemolytic activities	EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY	2017
Peptidomic analysis of skin secretions of the mexican burrowing toad Rhinophrynus dorsalis (rhinophrynidae): insight into the origin of host-defense peptides within the pipidae and characterization of a proline-arginine-rich peptide	PEPTIDES	2017
Rational modification of a dendrimeric peptide with antimicrobial activity: Consequences on membrane-binding and biological properties	AMINO ACIDS	2016
Bacillomycin d and its combination with amphotericin b: promising antifungal compounds with powerful antibiofilm activity and wound-healing potency	JOURNAL OF APPLIED MICROBIOLOGY	2016
NMR structure and binding of esculentin-1a (1-21)NH2 and its diastereomer to lipopolysaccharide: correlation with biological functions	BIOCHIMICA ET BIOPHYSICA ACTA-BIOMEMBRANES	2016
Antimicrobial peptides and wound healing: biological and therapeutic considerations	EXPERIMENTAL DERMATOLOGY	2016
Editorial (Thematic Issue: Antimicrobial Peptides in Medicinal Chemistry: Advances and Applications)	CURRENT TOPICS IN MEDICINAL CHEMISTRY	2016
Naturally occurring peptides from Rana temporaria: antimicrobial properties and more	CURRENT TOPICS IN MEDICINAL CHEMISTRY	2016
Esculentin-1a-derived peptides promote clearance of pseudomonas aeruginosa internalized in bronchial cells of cystic fibrosis patients and lung cell migration: Biochemical properties and a plausible mode of action	ANTIMICROBIAL AGENTS AND CHEMOTHERAPY	2016
Purification, conformational analysis, and properties of a family of tigerinin peptides from skin secretions of the crowned bullfrog hoplobatrachus occipitalis	JOURNAL OF NATURAL PRODUCTS	2016
Esculentin-1a(1-21) and its diastereomer: frog skin-derived peptides with anti-Pseudomonal activities	REGPEP 2016 Iternational Regulatory Peptide Society Program and Abstracts	2016
Effetti della coniugazione del peptide antimicrobico Esc(1-21) a nanoparticelle di oro		2016

ERC

LS1
LS6_1
LS6_8
LS6_9

KET

Life-science technologies & biotechnologies

Interessi di ricerca

My research interest is mainly focused on the structure-function characterization of amphibian skin-derived antimicrobial peptides (AMPs) or de-novo designed analogues for the development of new therapeutic agents against the worldwide alarming threat of multidrug-resistant infections. In contrast with traditional antibiotics, amphibian skin AMPs have: (i) a rapid killing mechanism based on the perturbation of the microbial plasma-membrane, causing irreparable damage that hardly induces resistance; (ii) an anti-biofilm activity and (iii) additional biological properties including the neutralization of the toxic effect of the bacterial lipopolysaccharide as well as the promotion of wound healing activity.

In the past years, a frog-skin derived peptide i.e. Esc(1-21) was found to display a significant in vivo efficacy in a mouse model of keratitis induced by the bacterium Pseudomonas aeruginosa. So far only a few in vivo experiments have provided signs of clinical benefit of AMPs against keratitis. At the same time, it was discovered how the presence of only two L-to D amino acids substitution within Esc(1-21) is sufficient to improve the peptide’s selectivity index, biostability, wound healing activity and in vivo therapeutic efficacy. In parallel, it was found that this selective epimerization can affect the peptide’s ability to interact with the bacterial lipopolysaccharide (LPS) or model membranes (liposomes) as well as with nucleotides (i.e. guanosine pentaphosphate, ppGpp) preventing biofilm formation. However, a key step for AMPs development is a proper delivery system to target them at the site of infection at effective concentration, with minimal off-target effects. In this context, by means of nanotechnology approaches, it was demonstrated how encapsulation of these peptides inside engineered biodegradable polymeric nanoparticles is an excellent strategy (i) to overcome lung barriers (i.e. the sticky mucus lying the airways epithelia, mostly in cystic fibrosis sufferers) that usually interfere with the antibiotic treatment and (ii) to prolong the antimicrobial efficacy of the encapsulated peptide.

Consistent with the above goals, the main objectives of my current scientific research include:

The development of new inhalable formulations to optimize the pulmonary delivery of peptides and to provide their controlled release over time;
The development of antimicrobial medical devices, such as peptide-immobilized contact lenses, to prevent microbial colonization of the lenses and the incidence of ocular surface infections.
The development of peptide-based nano-formulations to apply locally in a suitable solution or using nanoparticulate systems, in order to accelerate wound-healing of the corneal/bronchial epithelium or the skin.
Design and characterization of peptide analogs for SAR studies

Finally, by using experimental conditions that allow both the determination of microbicidal activity and the measurement of peptide/membrane association directly in bacteria, the gap between biological and physicochemical studies was filled and the amount of cell-bound peptide molecules needed for killing a bacterium for identified. Studies aimed at assessing the exact site of association of peptides to bacterial cells are in progress.

Keywords

antimicrobial peptides

antibiotic resistance

antibiotic delivery

cystic fibrosis

biomembranes

Bacterial Infections

corneal wound healing

anti-inflammatory agents

Progetti di Ricerca

Gruppi di ricerca - Responsabile

Bioactive Peptides