Your search keyword '"Di Paolo, Antonello"' showing total 15 results

1. Dihydropyrimidine dehydrogenase gene variants for predicting grade 4-5 fluoropyrimidine-induced toxicity: FUSAFE individual patient data meta-analysis.

Author

Le Teuff, Gwénaël, Cozic, Nathalie, Boyer, Jean-Christophe, Boige, Valérie, Diasio, Robert B., Taieb, Julien, Meulendijks, Didier, Palles, Claire, Schwab, Matthias, Deenen, Maarten, Largiadèr, Carlo R., Marinaki, Anthony, Jennings, Barbara A., Wettergren, Yvonne, Di Paolo, Antonello, Gross, Eva, Budai, Barna, Ackland, Stephen P., van Kuilenburg, André B. P., and McLeod, Howard L.

Abstract

Background: Dihydropyrimidine dehydrogenase (DPD) deficiency is the main known cause of life-threatening fluoropyrimidine (FP)-induced toxicities. We conducted a meta-analysis on individual patient data to assess the contribution of deleterious DPYD variants *2A/D949V/*13/HapB3 (recommended by EMA) and clinical factors, for predicting G4-5 toxicity. Methods: Study eligibility criteria included recruitment of Caucasian patients without DPD-based FP-dose adjustment. Main endpoint was 12-week haematological or digestive G4-5 toxicity. The value of DPYD variants *2A/p.D949V/*13 merged, HapB3, and MIR27A rs895819 was evaluated using multivariable logistic models (AUC). Results: Among 25 eligible studies, complete clinical variables and primary endpoint were available in 15 studies (8733 patients). Twelve-week G4-5 toxicity prevalence was 7.3% (641 events). The clinical model included age, sex, body mass index, schedule of FP-administration, concomitant anticancer drugs. Adding *2A/p.D949V/*13 variants (at least one allele, prevalence 2.2%, OR 9.5 [95%CI 6.7–13.5]) significantly improved the model (p < 0.0001). The addition of HapB3 (prevalence 4.0%, 98.6% heterozygous), in spite of significant association with toxicity (OR 1.8 [95%CI 1.2–2.7]), did not improve the model. MIR27A rs895819 was not associated with toxicity, irrespective of DPYD variants. Conclusions: FUSAFE meta-analysis highlights the major relevance of DPYD *2A/p.D949V/*13 combined with clinical variables to identify patients at risk of very severe FP-related toxicity. [ABSTRACT FROM AUTHOR]

Published

2024

2. Daptomycin Plasma and CSF Levels in Patients with Healthcare-Associated Meningitis.

Author

Piva, S., Di Paolo, Antonello, Galeotti, Laura, Ceccherini, Francesco, Cordoni, Francesco, Signorini, Liana, Togni, Tommaso, De Nicolò, Amedeo, Rasulo, Frank A., Fagoni, Nazzareno, Latronico, N., and D'Avolio, Antonio

Subjects

*MENINGITIS, *CENTRAL nervous system, *CEREBROSPINAL fluid

Abstract

Background: There are currently few data concerning the cerebrospinal fluid (CSF) penetration of daptomycin in patients with healthcare-associated meningitis. This study aims (1) to better characterize the pharmacokinetics of daptomycin in humans during a 7-day intravenous (IV) therapy course, and (2) to study the penetration of daptomycin in the CSF after IV infusion at the dose of 10 mg/kg.Results: In this prospective observational study, we enrolled nine patients with an implanted external ventricular drainage and a diagnosis of a healthcare-associated meningitis. Daptomycin was administered at 10 mg/kg for a maximum of 7 days. The pharmacokinetic of daptomycin was studied using a two-compartment population/pharmacokinetic (POP/PK) model and by means of a nonlinear mixed effects modeling approach. A large inter-individual variability in plasma area under the curve (Range: 574.7-1366.3 h mg/L), paralleled by high-peak plasma concentration (Cmax) (all values > 60 mg/L), was noted. The inter-individual variability of CSF-AUC although significant (range: 1.17-6.81 h mg/L) was narrower than previously reported and with a late occurrence of CSF-Cmax (range: 6.04-9.54 h). The terminal half-life between plasma and CSF was similar. tmax values in CSF did not show a high inter-individual variability, and the fluctuations of predicted CSF concentrations were minimal. The mean value for daptomycin penetration obtained from our model was 0.45%.Conclusions: Our POP/PK model was able to describe the pharmacokinetics of daptomycin in both plasma and CSF, showing that daptomycin (up to 7 days at 10 mg/kg) has minimal penetration into central nervous system. Furthermore, the observed variability of AUC, tmax and predicted concentration in CSF was lower than what previously reported in the literature. Based on the present findings, it is unlikely that daptomycin could reach CSF concentrations high enough to have clinical efficacy; this should be tested in future studies. [ABSTRACT FROM AUTHOR]

Published

2019

3. Generic Substitution of Orphan Drugs for the Treatment of Rare Diseases: Exploring the Potential Challenges.

Author

Di Paolo, Antonello and Arrigoni, Elena

Subjects

*CHRONIC diseases, *ORPHAN drugs, *MEDICAL care costs, *MEDICAL prescriptions, *RARE diseases, *SYSTEMATIC reviews, *EARLY intervention (Education), *ECONOMICS, *THERAPEUTICS

Abstract

Generic drugs are important components of measures introduced by healthcare regulatory authorities to reduce treatment costs. In most patients and conditions the switch from a branded drug to its generic counterpart is performed with no major complications. However, evidence from complex diseases suggests that generic substitution requires careful evaluation in some settings and that current bioequivalence criteria may not always be adequate for establishing the interchangeability of branded and generic products. Rare diseases, also called orphan diseases, are a group of heterogeneous diseases that share important characteristics: in addition to their scarcity, most are severe, chronic, highly debilitating, and often present in early childhood. Finding a treatment for a rare disease is challenging. Thanks to incentives that encourage research and development programs in rare diseases, several orphan drugs are currently available. The elevated cost of orphan drugs is a highly debated issue and a cause of limited access to treatment for many patients. As patent protection and the exclusivity period of several orphan drugs will expire soon, generic versions of orphan drugs should reach the market shortly, with great expectations about their impact on the economic burden of rare diseases. However, consistent with other complex diseases, generic substitution may require thoughtful considerations and may be even contraindicated in some rare conditions. This article provides an overview of rare disease characteristics, reviews reports of problematic generic substitution, and discusses why generic substitution of orphan drugs may be challenging and should be undertaken carefully in rare disease patients. [ABSTRACT FROM AUTHOR]

Published

2018

4. The Resistance to Tyrosine Kinase Inhibitors in Chronic Myeloid Leukemia: An Overview.

Author

Galimberti, Sara, Baratè, Claudia, Petrini, Mario, Focosi, Daniele, Arrigoni, Elena, Danesi, Romano, and Di Paolo, Antonello

Published

2016

5. Association of the hOCT1/ABCB1 genotype with efficacy and tolerability of imatinib in patients affected by chronic myeloid leukemia.

Author

Galeotti, Laura, Ceccherini, Francesco, Domingo, Dario, Laurino, Marco, Polillo, Marialuisa, Di Paolo, Antonello, Baratè, Claudia, Fava, Carmen, D'Avolio, Antonio, Cervetti, Giulia, Guerrini, Francesca, Fontanelli, Giulia, Ciabatti, Elena, Grassi, Susanna, Arrigoni, Elena, Danesi, Romano, Petrini, Mario, Cornolti, Fulvio, Saglio, Giuseppe, and Galimberti, Sara

Subjects

TREATMENT of chronic myeloid leukemia, CHRONIC myeloid leukemia, IMATINIB, ORGANIC cation transporters, DRUG efficacy, DRUG toxicity, SINGLE nucleotide polymorphisms, PATIENTS, ANTINEOPLASTIC agents, EDEMA, FACTOR analysis, GENETIC polymorphisms, GLYCOPROTEINS, HUMAN reproduction, PHARMACOGENOMICS, PROGNOSIS, PROTEINS, MUSCLE cramps, GENOTYPES

Abstract

Purpose: The present study was aimed at investigating whether imatinib pharmacogenetics is related to its pharmacodynamics in patients affected by chronic myeloid leukemia.Methods: Through a procedure based on a sequence of classical statistics methods, we investigated the possible relationships between treatment efficacy/tolerability and combinations of time-independent variables as gender and genetic covariates in the form of single nucleotide polymorphisms (SNPs) or combinations thereof. Moreover, since the drug tolerability has a strong incidence on the discontinuation of the therapy, we investigated whether the time of manifestation of the most frequent toxic effects can be related to time-independent patients' characteristics or not.Results: We found that a combination of two polymorphisms, namely hOCT1 c.480C>G (rs683369) and ABCB1 c.3435C>T (rs1045642), seems to play the role of predictor for imatinib in both efficacy and toxicity. Furthermore, the time of manifestation of edema toxicity is found to be associated to a combination of gender and ABCB1 c.3435C>T, whereas the time of manifestation of cramp toxicity appears related to gender.Conclusions: The novelty of this study is dual: the achievement of results that potentially have a significant clinical interest and the demonstration that the adoption of composed covariates may represent a unique tool to study different aspects of the treatment with imatinib. [ABSTRACT FROM AUTHOR]

Published

2017

6. Pharmacogenetics of Angiogenesis.

Author

Bocci, Guido, Pasqualetti, Giuseppe, Di Paolo, Antonello, Crea, Francesco, Del Tacca, Mario, and Danesi, Romano

Abstract

Angiogenesis is a complex cascade of events involving extensive interplay between cells, soluble factors, and extracellular matrix components. Soluble factors including cytokines and growth factors have multifaceted stimulatory or inhibitory roles, thereby finely tuning the process. The angiogenic potential of tumors was initially demonstrated in animal models, and it is now recognized that angiogenesis not only precedes tumor growth but is also necessary for metastasis. Vascular endothelial growth factor (VEGF) plays a central role in prostate angiogenesis. Genetic variability of VEGF involves mainly the untranslated region of the gene and may be associated with increased VEGF transcription and protein expression. Indeed, the -1154G>A polymorphism increases VEGF transcription and has been associated with significantly increased risk of prostate cancer. Hypoxia inducible factor-1α (HIF-1α) is a transcription factor overexpressed in early stage prostate cancer; through its binding to hypoxic responsive elements, it activates the transcription of a wide variety of genes as a part of the cellular response to hypoxia, including VEGF, and potentially plays a key role in prostate cancer development and response to antiangiogenic drugs. Therefore, angiogenesis-related genes seem to have an important role in prostate cancer risk and aggressiveness, thus influencing the outcome of antiangiogenic treatments and survival of patients. [ABSTRACT FROM AUTHOR]

Published

2010

7. EGFR ligands as pharmacodynamic biomarkers in metastatic colorectal cancer patients treated with cetuximab and irinotecan.

Author

Loupakis, Fotios, Cremolini, Chiara, Fioravanti, Anna, Orlandi, Paola, Salvatore, Lisa, Masi, Gianluca, Schirripa, Marta, Di Desidero, Teresa, Antoniotti, Carlotta, Canu, Bastianina, Faviana, Pinuccia, Sensi, Elisa, Lupi, Cristiana, Fontanini, Gabriella, Basolo, Fulvio, Di Paolo, Antonello, Danesi, Romano, Falcone, Alfredo, and Bocci, Guido

Abstract

This study was conducted to describe the modulation of plasma epidermal growth factor receptor (EGFR) ligands in EGFR-positive metastatic colorectal cancer (mCRC) patients during treatment with cetuximab and irinotecan and to explore the clinical implication of plasma levels' variations as potential biomarkers of benefit. Plasma amphiregulin (AR), epidermal growth factor (EGF), transforming growth factor-α, and heparin binding-EGF were assessed by ELISA in 45 chemorefractory mCRC patients, treated with cetuximab and irinotecan. Plasma levels were measured before and 1 h after the first administration of cetuximab, before and 1 h after the second administration, and before the third and the fifth cycles. KRAS and BRAF mutational status were determined. EGFR ligands' levels were differently modulated according to tumor KRAS and BRAF mutational status. In KRAS wild-type patients ( n = 34), AR and EGF early increased and higher increases were significantly associated with worse clinical outcome. By adopting a specific cut-off value, patients with higher levels of AR 1 h after the first administration had significantly worse response rate, progression free survival, and overall survival. This hypothesis-generating study shows that EGFR ligands are significantly modulated by cetuximab plus irinotecan according to KRAS and BRAF mutational status, and they warrant further investigation as pharmacodynamic markers of resistance to anti-EGFRs. [ABSTRACT FROM AUTHOR]

Published

2014

8. Clinical Pharmacokinetics of Antibacterials in Cerebrospinal Fluid.

Author

Di Paolo, Antonello, Gori, Giovanni, Tascini, Carlo, Danesi, Romano, and Del Tacca, Mario

Subjects

*PHARMACOKINETICS, *ANTIBACTERIAL agents, *CEREBROSPINAL fluid, *MULTIDRUG resistance, *CENTRAL nervous system diseases, *THERAPEUTICS, *CEPHALOSPORINS, *CARBAPENEMS

Abstract

In the past 20 years, an increased discrepancy between new available antibacterials and the emergence of multidrug-resistant strains has been observed. This condition concerns physicians involved in the treatment of central nervous system (CNS) infections, for which clinical and microbiological success depends on the rapid achievement of bactericidal concentrations. In order to accomplish this aim, the choice of drugs is based on their disposition toward the cerebrospinal fluid (CSF), which is influenced by the physicochemical characteristics of antibacterials. A reduced distribution into CSF has been documented for beta-lactams, especially cephalosporins and carbapenems, on the basis of their hydrophilic nature. However, they represent a cornerstone of the majority of combined therapeutic schemes for their ability to achieve bactericidal concentrations, especially in the presence of inflamed meninges. The good tolerability of beta-lactams makes possible high daily dose intensities, which may be associated with increased probability of cure. Furthermore, the adoption of continuous infusion seems to be a fruitful option. Fluoroquinolones, namely moxifloxacin, and antituberculosis drugs, together with the agents such as linezolid, reach the highest CSF/plasma concentration ratio, which is greater than 0.8, and for most of these drugs it is near 1. For all drugs that are currently used for the treatment of CNS infections, the evaluation of pharmacokinetic/pharmacodynamic parameters, on the basis of dosing regimens and their time-dependent or concentration-dependent pattern of bacterial killing, remains an important aspect of clinical investigation and medical practice. [ABSTRACT FROM AUTHOR]

Published

2013

9. The pharmacological bases of the antiangiogenic activity of paclitaxel.

Author

Bocci, Guido, Di Paolo, Antonello, and Danesi, Romano

Subjects

PACLITAXEL, ANTINEOPLASTIC agents, NEOVASCULARIZATION, CELL migration, ENDOTHELIAL cells, VASCULAR endothelial growth factors, GENE expression

Abstract

In the mid 1990s, researchers began to investigate the antiangiogenic activity of paclitaxel as a possible additional mechanism contributing to its antineoplastic activity in vivo. In the last decade, a number of studies showed that paclitaxel has antiangiogenic activity that could be ascribed to the inhibition of either tubule formation or cell migration, and to an antiproliferative effect towards activated endothelial cells. Furthermore, paclitaxel was shown to downregulate VEGF and Ang-1 expression in tumor cells, and to increase the secretion of TSP-1 in the tumor microenvironment. Moreover, the new pharmaceutical formulations of paclitaxel (such as liposome-encapsulated paclitaxel, ABI-007, and paclitaxel entrapped in emulsifying wax nanoparticles) enhanced the in vivo antiangiogenic activity of the drug. Thus, the preclinical data of paclitaxel may be exploited to implement a novel and rational therapeutic strategy to control tumor progression in patients. [ABSTRACT FROM AUTHOR]

Published

2013

10. Clinical, pharmacokinetic and pharmacodynamic evaluations of metronomic UFT and cyclophosphamide plus celecoxib in patients with advanced refractory gastrointestinal cancers.

Author

Allegrini, Giacomo, Di Desidero, Teresa, Barletta, Maria, Fioravanti, Anna, Orlandi, Paola, Canu, Bastianina, Chericoni, Silvio, Loupakis, Fotios, Di Paolo, Antonello, Masi, Gianluca, Fontana, Andrea, Lucchesi, Sara, Arrighi, Giada, Giusiani, Mario, Ciarlo, Andrea, Brandi, Giovanni, Danesi, Romano, Kerbel, Robert, Falcone, Alfredo, and Bocci, Guido

Subjects

PHARMACOKINETICS, PHARMACODYNAMICS, CYCLOPHOSPHAMIDE, CELECOXIB, GASTROINTESTINAL cancer treatment, DRUG therapy, VASCULAR endothelial growth factors

Abstract

Aims: To evaluate UFT and cyclophosphamide (CTX) based metronomic chemotherapy plus celecoxib (CXB) for the treatment of patients with heavily pre-treated advanced gastrointestinal malignancies. Methods: Thirty-eight patients received 500 mg/mq CTX i.v bolus on day 1 and, from day 2, 50 mg/day CTX p.o. plus 100 mg/twice a day UFT p.o. and 200 mg/twice a day CXB p.o. Tegafur, 5-FU, 5-FUH, GHB and uracil pharmacokinetics were assessed. Plasma vascular endothelial growth factor (VEGF), soluble VE-cadherin (sVE-C) and thrombospondin-1 (TSP-1) levels were detected by ELISA and real-time PCR of CD133 gene expression on peripheral blood mononuclear cell was also performed. Results: Seventeen patients (45%) obtained stable disease (SD) with a median duration of 5.8 ms (range, 4.2-7.4). Median progression free survival (PFS) and overall survival (OS) were 2.7 ms (95% CI, 1.6-3.9 ms) and 7.1 ms (95% CI, 4.3-9.9 ms), respectively. No toxicities of grade >1 were observed. Pharmacokinetics of 27 patients (13/14, SD/progressive disease, PD) after the first treatment of UFT revealed that 5-FU AUC and C values greater than 1.313 h × μg/ml and 0.501 μg/ml, respectively, were statistically correlated with stabilization of disease and prolonged PFS/OS. VEGF and sVE-C plasma levels were greater in the PD group when compared to SD group. CD133 expression increased only in the PD patients. Conclusion: Metronomic UFT and CTX with CXB in heavily pre-treated gastrointestinal patients were well tolerated and associated with interesting activity. Potential predictive pharmacokinetic parameters and pharmacodynamic biomarkers have been found. [ABSTRACT FROM AUTHOR]

Published

2012

11. Pharmacological Issues of Linezolid.

Author

Di Paolo, Antonello, Malacarne, Paolo, Guidotti, Emanuele, Danesi, Romano, and Del Tacca, Mario

Subjects

*PHARMACOLOGY, *GRAM-positive bacterial infections, *PHARMACOKINETICS, *GLYCOPEPTIDES, *METHICILLIN-resistant staphylococcus aureus, *STAPHYLOCOCCUS aureus infections, *ANTIBACTERIAL agents, *BACTERIAL disease treatment, *THERAPEUTICS

Abstract

Linezolid is the first oxazolidinone agent introduced into clinical practice for use against Gram-positive bacteria that are resistant to β-lactams and glycopeptides, including methicillin (meticillin)-resistant Staphylococcus aureus (MRSA) and vancomycin-resistant enterococci (VRE). An optimal antibacterial effect is achieved when plasma drug concentrations are above the minimum inhibitory concentration (MIC) [T>MIC] for the entire length of treatment and the ratio between the area under the plasma concentration-time curve (AUC) and the MIC (AUC/MIC) is greater than 100, as is most commonly obtained with administration of the standard dosage of linezolid 600 mg twice daily. A wide tissue distribution, including the CNS and respiratory tract, nearly linear pharmacokinetics and good tolerability are additional characteristics of linezolid. However, variability in the drug pharmacokinetics associated with clinical conditions (e.g. sepsis, burn injuries, end-stage renal disease, cystic fibrosis), haemodialysis and/or young age may lower the T>MIC and the AUC/MIC ratio, thus impairing both antibacterial activity and prevention of mutants. In most cases, changes in the dosage or in the schedule of administration (e.g. an additional [third] daily dose) may improve the effectiveness of linezolid. It is worth noting that linezolid could affect its own metabolism as a result of protein synthesis inhibition in mitochondria, and this could lead to high plasma concentrations and an increased risk of non-negligible toxicities. The latter may be reported during long-term administration of linezolid or in the presence of some pathological conditions (e.g. renal disease or kidney transplantation) associated with high plasma drug concentrations. Therefore, treatment optimization should be considered a requirement for more effective and tolerable use of the drug, particularly in special populations. [ABSTRACT FROM AUTHOR]

Published

2010

12. Irinotecan in combination with thalidomide in patients with advanced solid tumors: a clinical study with pharmacodynamic and pharmacokinetic evaluation.

Author

Allegrini, Giacomo, Di Paolo, Antonello, Cerri, Elisa, Cupini, Samanta, Amatori, Federica, Masi, Gianluca, Danesi, Romano, Marcucci, Lorenzo, Bocci, Guido, del Tacca, Mario, and Falcone, Alfredo

Subjects

*THALIDOMIDE, *TUMORS, *PHARMACODYNAMICS, *PHARMACOKINETICS, *COLON cancer, *ANTINEOPLASTIC agents, *BRAIN tumors, *CAMPTOTHECIN, *CLINICAL trials, *COMPARATIVE studies, *DIARRHEA, *DRUG administration, *HYPERSOMNIA, *INTRAVENOUS therapy, *RESEARCH methodology, *MEDICAL cooperation, *METASTASIS, *ORAL drug administration, *RESEARCH, *TIME, *EVALUATION research, *TREATMENT effectiveness

Abstract

Purpose: Recent clinical studies have demonstrated a reduction of irinotecan (CPT-11) gastrointestinal toxicities when the CPT-11 is administered in combination with thalidomide in patients with diagnosis of colorectal cancer. The main purpose of this study was to investigate possible interactions between CPT-11 pharmacokinetics and thalidomide to explain the previously described gastrointestinal toxicity reduction. Methods: In our clinical trial, advanced cancer patients were treated with CPT-11 on a dose of 350 mg/m2 at day 1 every 3 weeks. Only at the first cycle, CPT-11 was administered in association with thalidomide on a dose of 400 mg/day given from day 1 to day 14. From the second cycle, the treatment was continued with irinotecan alone at the same dose. Pharmacokinetics analysis of irinotecan and its metabolites, SN-38 and SN-38-glucuronide, were performed at the first and second cycle. Results: A total of 19 patients entered the study. The pharmacokinetic analysis were performed on 16 patients. Pharmacokinetic data suggested a decreased metabolism of irinotecan into SN-38 and SN-38-glucuronide when it was administered with thalidomide. Indeed, area under the time–concentration curve (AUC) of SN-38 was significantly lower at the first cycle than the second cycle (0.99±0.45 h×μg/ml vs 1.34±0.65, respectively, P=0.027) whereas AUC of irinotecan and SN-38-glucuronide were higher at first cycle than second cycle (34.53±11.38 h×µg/ml vs. 28.42±12.23 h×µg/ml, P=0.064 and 2.39±1.21 h(μg/ml vs. 1.86±1.11 h×μg/ml, P=0.018, respectively). Conclusions: Our study demonstrates a significant decreased metabolism of CPT-11 into the active metabolite SN-38 when CPT-11 is administered in association with thalidomide. These observations strongly suggest an interaction of thalidomide with CPT-11 metabolism and, at least in part, it might explain the previously described improvement in tolerability. [ABSTRACT FROM AUTHOR]

Published

2006

13. Metabolism of 6-mercaptopurine in the erythrocytes, liver, and kidney of rats during multiple-dose regimens.

Author

Innocenti, Federico, Danesi, Romano, Bocci, Guido, Fogli, Stefano, Di Paolo, Antonello, and Del Tacca, M.

Abstract

Purpose: To describe the metabolism of 6-mercaptopurine (6-MP) in erythrocytes and tissues of rats after repeated administration of 6-MP at two dose levels and to provide evidence that in vivo modulation of 6-MP anabolism can be obtained by simultaneous treatment with ribavirin or hydroxyurea, two inhibitors of enzymes involved in the bioactivation of 6-MP to the active 6-thioguanine nucleotides (6-TGN). Methods: Rats were treated i.p. with 6-MP at 12.5 and 25 mg/kg daily for 12 days and erythrocyte, liver, and kidney levels of 6-mercaptopurine nucleotides (6-MPN) and 6-TGN were investigated during the accumulation phase and for 50 days after the end of treatment. In combination studies, ribavirin at 75 and 100 mg/kg per day (for 6-MP, 25 and 12.5 mg/kg per day) or hydroxyurea at 200 mg/kg per day were given i.p. for 12 days. The measurements of thionucleotide levels in rat samples were performed by high-pressure liquid chromatography (HPLC). Results: The maximal concentration (Cmax) and the area under the concentration versus time curve (AUC) of 6-MPN and 6-TGN in erythrocytes and tissues increased significantly after the administration of 6-MP at 25 mg/kg per day as compared with 12.5 mg/kg per day. In particular, the Cmax and AUC of 6-TGN in erythrocytes of rats treated with 6-MP at 25 mg/kg per day were approximately 5-fold higher than the 6-TGN values observed following treatment at 12.5 mg/kg per day. Moreover, 6-TGN levels in erythrocytes were significantly higher than those of 6-MPN (910.9 ± 53.1 and 286.8 ± 23.4 pmol/8 × 108 cells for 6-TGN and 6-MPN, respectively, P < 0.05) after treatment with 6-MP at 25 mg/kg per day. The administration of ribavirin, an inhibitor of inosine monophosphate dehydrogenase, in association with 6-MP increased the amount of 6-MPN detected in erythrocytes and tissues while reducing 6-TGN levels in samples. The production and accumulation of 6-MPN and 6-TGN were increased in erythrocytes and tissues by hydroxyurea, an inhibitor of ribonucleotide reductase. Finally, a significant correlation between thionucleotide concentrations and erythrocyte counts was observed. Conclusion: The overall results demonstrate that 6-MP is actively metabolized in rats and that its biotransformation can be modulated by agents acting on enzymes of the purine metabolism, resulting in significant changes in erythrocyte and tissue levels of 6-MPN and 6-TGN. These findings provide evidence that the rat is a suitable model for investigation of the metabolism of 6-MP and its possible pharmacologic modulation. [ABSTRACT FROM AUTHOR]

Published

1999

14. Inhibitory effect of suramin in rat models of angiogenesis in vitro and in vivo.

Author

Bocci, Guido, Danesi, Romano, Benelli, Umberto, Innocenti, Federico, Di Paolo, Antonello, Fogli, Stefano, and Del Tacca, Mario

Abstract

The aim of the present study was to test the ability of the chemotherapeutic agent suramin to inhibit angiogenesis in experimental models in vitro and in vivo. In the culture of rat aortic rings on fibronectin, suramin dose-dependently inhibited vascular cell growth, achieving the maximal effect (mean − 88% versus controls, P < 0.05) at 400 μg/ml. Image analysis showed that suramin could inhibit microvessel sprouting in fibrin from rat aortic rings as evaluated by the ratio between the cellular area and the mean gray value of the sample (sprouting index); suramin at 50 μg/ml significantly reduced the sprouting index from the control value of 0.35 ± 0.04 to 0.14 ± 0.02 mm2/gray level ( P < 0.05). Likewise, the area occupied by cells was 19.2 ± 1.8 mm2 as compared with 41.8 ± 4.2 mm2 in controls ( P < 0.05). In the rat model of neovascularization induced in the cornea by chemical injury, suramin at 1.6 mg/eye per day reduced the length of blood vessels (0.7 ± 0.1 mm as compared with 1.5 ± 0.1 mm in controls, P < 0.05). In the same model the ratio between the area of blood vessels and the total area of the cornea (area fraction score) was decreased by suramin from 0.19 ± 0.02 in controls to 0.03 ± 0.003 ( P < 0.05). Suramin given i.p. at 30 mg/kg per day markedly inhibited the neovascularization induced in the rat mesentery by compound 48/80 or conditioned medium from cells secreting the angiogenic protein fibroblast growth factor-3 (FGF-3). The area fraction score in control rats treated with compound 48/80 was 0.31 ± 0.03, and this was reduced to 0.07 ± 0.01 by suramin ( P < 0.05). After i.p. administration of FGF-3 the area fraction score was reduced by suramin from 0.29 ± 0.03 to 0.05 ± 0.01 ( P < 0.05). These results provide evidence that suramin exerts inhibitory effects on angiogenesis in both in vitro and in vivo models. [ABSTRACT FROM AUTHOR]

Published

1999

15. Oral administration of gentamicin for prophylaxis of KPC-producing Klebsiella pneumoniae gut colonization in patients treated with a novel parenchymal-sparing liver surgery: the GEN Gut study.

Author

Tascini, Carlo, Urbani, Lucio, Sbrana, Francesco, Forfori, Francesco, Licitra, Gabriella, Leoni, Chiara, Balestri, Riccardo, Rossi, Elisabetta, Fortunato, Simona, Leonildi, Alessandro, Puccini, Marco, Di Paolo, Antonello, Ripoli, Andrea, Colombatto, Piero, Menichetti, Francesco, and Buccianti, Piero

Subjects

GENTAMICIN, KLEBSIELLA pneumoniae, BETA-lactamase inhibitors, HEPATECTOMY, ORAL drug administration, ANTIBIOTICS, LIVER surgery, GUT microbiome, KLEBSIELLA infections, CHEMOPREVENTION, DIGESTIVE organ surgery, KLEBSIELLA, PILOT projects, PREVENTION, THERAPEUTICS

Abstract

The article discusses the authors' plan to initiate the oral administration of gentamicin in a multidisciplinary round table to avoid Klebsiella pneumoniae producing KPC-type beta-lactamase (KPC-Kp) gut colonization in patients undergoing hepatectomy. It suggests a randomized controlled trial with extended microbiologial follow-up to validate the hypothesis that oral prophylaxis with gentamicin is effective in preventing KPC-Kp colonization in patients with complex abdominal surgery.

Published

2016