Your search keyword '"C. Di Bello"' showing total 5 results

1. Total synthesis of horse heart cytochrome c. Preparation and characterization of the (1-66)apofragment.

Author

Di Bello C and Gozzini L

Subjects

Amino Acid Sequence, Animals, Antibodies, Monoclonal, Apoproteins drug effects, Apoproteins immunology, Chymotrypsin pharmacology, Cytochrome c Group drug effects, Cytochrome c Group immunology, Horses, Molecular Sequence Data, Myocardium chemistry, Peptide Fragments chemical synthesis, Trypsin pharmacology, Apoproteins chemical synthesis, Cytochrome c Group chemical synthesis

Abstract

A peptide corresponding to the native (1-66) sequence of horse heart cytochrome c has been synthesized by stepwise automated solid-phase methods on PAM resin. The course of the synthesis has been monitored by several analytical methods including quantitative ninhydrin and Edman degradation. After HF cleavage, the peptide has been purified by a combination of semipreparative ion-exchange and RP-HPLC. The homogeneity of the purified synthetic peptide has been determined by different criteria including HPLC, amino-acid composition, electrophoresis, antibody binding, tryptic and chymotryptic peptide mapping. After deprotection of the Acm-Cys residues and CNBr cleavage of the Met65-Glu66 peptide bond with simultaneous transformation of the Met65 residue into the activated C-terminal [Hse65]lactone, this purified synthetic peptide has been utilized for conformation-assisted joining experiments in combination with synthetic (66-104) to produce fully synthetic [Hse65]apocytochrome c. This latter, after mitochondria-mediated stereospecific heme insertion, has given a functional molecule corresponding to native horse heart holocytochrome c.

Published

1993

2. Solid-phase synthesis of the native sequence of horse heart cytochrome c-(66-104)-nonatriacontapeptide and of a C-terminal carboxyamide analog selectively modified at Met-80.

Author

di Bello C, Tonellato M, Lucchiari A, Buso O, Gozzini L, and Vita C

Subjects

Amino Acid Sequence, Animals, Horses, Molecular Sequence Data, Cytochrome c Group chemical synthesis, Myocardium enzymology, Peptide Fragments chemical synthesis

Abstract

The peptide corresponding to the (66-104) sequence of horse heart cytochrome c and its carboxyamide analog, selectively modified at the critical Met80 residue, have been synthesized by stepwise solid-phase methods on PAM and BHA resins respectively. The correctness of the growing peptide chain as well as the homogeneity of the final products have been monitored by several analytical methods including quantitative Edman degradation. After HF cleavage both peptides were purified by semipreparative HPLC. The overall yields were 24% for the native (66-104) and 10% for the carboxyamide analog. The homogeneity of the purified synthetic peptides have been determined by different criteria including HPLC, amino acid composition, Edman degradation, electrophoresis, and tryptic peptide mapping. The synthetic fragments have been utilized for preliminary semisynthesis experiments with the native [Hse greater than 65] (1-65)H heme-sequence.

Published

1990

3. Synthesis, purification and conformational studies on enkephalin derivatives containing gamma-amino-n-butyric acid.

Author

Di Bello C, Andini S, Ferrara L, Napolitano R, and Paolillo L

Subjects

Chromatography, High Pressure Liquid, Magnetic Resonance Spectroscopy, Models, Molecular, Protein Conformation, Structure-Activity Relationship, Enkephalins chemical synthesis, gamma-Aminobutyric Acid

Abstract

The solid-phase synthesis of several analogs of enkephalin containing gamma-amino-butyric acid is reported. Synthetic strategies, purification methods, chemical and physicochemical characterization are discussed. The n.m.r. data suggest for some of the analogs structural features similar to the opioids.

Published

1982

4. Solid-phase synthesis of bombesin by continuous flow procedure using Fmoc-amino acids.

Author

Scolaro B, Gozzini L, Rocchi R, and Di Bello C

Subjects

Ammonia, Bombesin isolation & purification, Hydrofluoric Acid, Amino Acids, Bombesin chemical synthesis, Fluorenes

Abstract

Bombesin has been synthesized by the continuous flow solid-phase procedure on the derivatized Kieselguhr-supported polydimethylacrylamide resin. Preformed Fmoc-amino acid symmetrical anhydrides (Met, Leu, and Arg) and Fmoc-amino acid active esters were used for amine acylation. The Mtr and the Pmc groups have been alternatively used for masking the side chain function of Arg-3. The progress of the synthesis was monitored by different analytical methods including quantitative solid-phase Edman degradation. Cleavage from the resin and simultaneous formation of the C-terminal amide function were achieved with a methanolic ammonia solution yielding indistinguishable crude peptides which have been purified by HPLC and fully characterized. Preliminary pharmacological experiments indicated that the activity of the synthetic peptides is similar to that previously measured for other synthetic bombesins. For comparison bombesin has also been prepared by solid-phase synthesis on 4-methyl benhydrylamine resin using the Boc chemistry. The results of the two strategies are discussed and compared.

Published

1989

5. Semisynthetic studies on bovine pancreatic ribonuclease.

Author

Di Bello C, Lucchiari A, Buso O, and Tonellato M

Subjects

Amino Acid Sequence, Animals, Arginine, Cattle, Indicators and Reagents, Ribonuclease, Pancreatic metabolism, Trypsin, Peptide Fragments chemical synthesis, Ribonuclease, Pancreatic chemical synthesis

Abstract

The S-peptide of the enzyme bovine pancreatic ribonuclease has been used as a model for covalent semisynthesis. Methods for side-chain protection, enzymatic cleavage of the peptide chain at the level of the single arginine-10 and for selective deprotection of the alpha-carboxyl function of this residue, have been examined. The partially protected [1-10] sequence has been coupled to a solid-phase generated [11-15] sequence attached to the polymer. After deblocking from the solid-support, the [1-15] semisynthetic peptide was complexed with native S-protein to give a complex with high biological activity.

Published

1984