Raffaella Garzia
Chiesi Farmaceutici S.p.A.
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Publication
Featured researches published by Raffaella Garzia.
International Journal of Pharmaceutics | 1999
Gaetano Brambilla; D. Ganderton; Raffaella Garzia; David Lewis; Brian John Meakin; Paolo Ventura
The inclusion of non-volatile components such as glycerol or polyethylene glycol in hydrofluoralkane (HFA) solution formulations for pressurised metered dose inhalers (pMDIs), greatly increases the particle size of the aerosol. Cloud characteristics can be further modulated by permuting this factor with the choice of propellant and the dimensions of the actuator, to give a chosen fine particle dose and particle diameter. This principle has been used to design solutions which closely match the performance of chlorofluorocarbon based suspension formulations containing beclomethasone dipropionate, budesonide and ipratropium bromide as assessed for pharmaceutical equivalence using the Andersen Cascade impactor.
PLOS ONE | 2012
Matthias Seehase; Jennifer J. P. Collins; Elke Kuypers; Reint K. Jellema; Daan R. M. G. Ophelders; Olga L. Ospina; Jesús Pérez-Gil; Federico Bianco; Raffaella Garzia; Roberta Razzetti; Boris W. Kramer
Background Respiratory distress syndrome in preterm babies is caused by a pulmonary surfactant deficiency, but also by its inactivation due to various conditions, including plasma protein leakage. Surfactant replacement therapy is well established, but clinical observations and in vitro experiments suggested that its efficacy may be impaired by inactivation. A new synthetic surfactant (CHF 5633), containing synthetic surfactant protein B and C analogs, has shown comparable effects on oxygenation in ventilated preterm rabbits versus Poractant alfa, but superior resistance against inactivation in vitro. We hypothesized that CHF 5633 is also resistant to inactivation by serum albumin in vivo. Methodology/Principal Findings Nineteen preterm lambs of 127 days gestational age (term = 150 days) received CHF 5633 or Poractant alfa and were ventilated for 48 hours. Ninety minutes after birth, the animals received albumin with CHF 5633 or Poractant alfa. Animals received additional surfactant if PaO2 dropped below 100 mmHg. A pressure volume curve was done post mortem and markers of pulmonary inflammation, surfactant content and biophysiology, and lung histology were assessed. CHF 5633 treatment resulted in improved arterial pH, oxygenation and ventilation efficiency index. The survival rate was significantly higher after CHF 5633 treatment (5/7) than after Poractant alfa (1/8) after 48 hours of ventilation. Biophysical examination of the surfactant recovered from bronchoalveolar lavages revealed that films formed by CHF 5633-treated animals reached low surface tensions in a wider range of compression rates than films from Poractant alfa-treated animals. Conclusions For the first time a synthetic surfactant containing both surfactant protein B and C analogs showed significant benefit over animal derived surfactant in an in vivo model of surfactant inactivation in premature lambs.
Archive | 1999
David Lewis; David Ganderton; Brian Meakin; Paolo Ventura; Gaetano Brambilla; Raffaella Garzia
Archive | 1999
Eva Bernini; Chiara Malvolti; Raffaella Garzia; Gaetano Brambilla; Paolo Chiesi
Archive | 1999
David Lewis; David Ganderton; Brian Meakin; Paolo Ventura; Gaetano Brambilla; Raffaella Garzia
Archive | 2002
Chiara Malvolti; Raffaella Garzia
Archive | 2003
David Lewis; Davis Ganderton; Brian Meakin; Paolo Ventura; Gaetano Brambilla; Raffaella Garzia
Archive | 2002
Chiara Malvolti; Raffaella Garzia
Archive | 2000
Chiara Malvolti; Raffaella Garzia; Gaetano Brambilla; Paolo Chiesi
Archive | 2008
David Lewis; David Ganderton; Brian Meakin; Paolo Ventura; Gaetano Brambilla; Raffaella Garzia