Giulia Melegaro scite author profile

Giulia Melegaro

5Publications

14Citation Statements Received

15Citation Statements Given

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Nerviano Medical Sciences

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Morpholinylanthracyclines: cytotoxicity and antitumor activity of differently modified derivatives

Ripamonti¹,

Capolongo²,

Melegaro³

et al. 1996

Invest New Drugs

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The relationship between different chemical modifications on morpholinylanthracyclines and their ability to overcome multidrug resistance (MDR) has been evaluated testing all compounds in vitro on LoVo and LoVo/DX human colon adenocarcinoma cells and in vivo disseminated P388 and P388/DX murine leukemias. Results obtained led us to the following conclusions: 1) the insertion of the morpholinyl or the methoxymorpholinyl group on position 3' of the sugar moiety confers the ability to overcome MDR in vitro and in vivo; conversely, 4' morpholinyl compounds are effective on MDR cells only in vitro and result inactive in vivo on DX-resistant leukemia; 2) all chemical modifications performed on 3' morpholinyl or methoxymorpholinyl derivatives, that is substitutions on the aglycone or on position 2 of the morpholino ring, do not interfere with the activity of the compounds: all derivatives present in fact the same efficacy on sensitive and resistant models. It is concluded that position 3' in the sugar moiety plays a crucial role in the ability of morpholinyl-anthracyclines to overcome MDR.

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Decreased tyrosine phosphorylation in tumour cells resistant to FCE 24517 (tallimustine)

Ciomei

Pastori²,

Capolongo³

et al. 1995

Br J Cancer

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Summary Resistance to FCE 24517 is not related to the emergence of any of the most frequently observed phenotypes. We have found that two resistant cell lines (L1210/24517 murine leukaemia and LoVo/24517 human colon adenocarcinoma) present congenital modifications in tyrosyl phosphatase and kinase activities. Moreover, the cytotoxic activity of FCE 24517 is increased in combination with a tyrosine phosphatase inhibitor and decreased in combination with protein kinase inhibitors, this being in agreement with the hypothesis that the activity of this drug is strictly dependent on the presence of tyrosine phosphorylated protein(s).

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Characterisation of a LoVo subline resistant to a benzoyl mustard derivative of distamycin A (FCE 24517)

Capolongo¹,

Melegaro²,

Broggini³

et al. 1993

Br J Cancer

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Human colon adenocarcinoma cells (LoVo) resistant to the new antitumor agent FCE 24517 [benzoyl-mustard derivative of distamycin A] (LoVo/24517) are resistant to the selecting agent and related molecules as well as to vinblastine, with marginal or no resistance to other antitumour drugs. Treatment with verapamil, tamoxifen, nicergoline or cyclosporin A only partially restores the activity of FCE 24517 against LoVo/24517 cells. Such results suggest that resistance mechanisms possible specific for this class of compounds are operating. Images Figure 2

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Reversal of Multidrug Resistance by New Dihydropyridines with Low Calcium Antagonist Activity

et al. 1994

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The clinical use of Ca++ antagonist agents as modulators of multidrug resistance is limited by their strong vasodilator activity. This study reports data obtained by testing a series of new 1,4 dihydropyridine derivatives (DHPs) for their in vitro resistance modulating activity and their Ca++ antagonist effect. All the tested DHPs are active to increase doxorubicin activity with dose modifying factor values ranging between 2 and 47 on P388/DX cells and 12 and 36 on LoVo/DX cells. Their resistance modulating action is exerted through an increase of DX intracellular level. The Ca++ antagonist activity of DHPs, evaluated as capacity to inhibit the KCl-induced contractions in isolated Guinea pig ileum strips, is not related to their resistance modulating activity. This finding makes it possible to select, for further in vivo evaluations, compounds IX, X and XI, which have strong ability to overcome multidrug resistance and low Ca++ antagonist effect.

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In vitro activity of novel sulphonic derivatives of distamicyn A

Mariani¹,

Paio²,

Ciomei³

et al. 1992

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Giulia Melegaro

Morpholinylanthracyclines: cytotoxicity and antitumor activity of differently modified derivatives

Decreased tyrosine phosphorylation in tumour cells resistant to FCE 24517 (tallimustine)

Characterisation of a LoVo subline resistant to a benzoyl mustard derivative of distamycin A (FCE 24517)

Reversal of Multidrug Resistance by New Dihydropyridines with Low Calcium Antagonist Activity

In vitro activity of novel sulphonic derivatives of distamicyn A

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