Gelatin Microspheres as a Pulmonary Delivery System: Evaluation of Salmon Calcitonin Absorption

Author:

Morimoto Kazuhiro1,Katsumata Hideyuki2,Yabuta Toshiyuki2,Iwanaga Kazunori2,Kakemi Masawo2,Tabata Yasuhiko3,Ikada Yoshito3

Affiliation:

1. Department of Pharmaceutics, Hokkaido College of Pharmacy, 7-1, Katsuraoka-cho, Otaru-city, Hokkaido 047–0264, Japan

2. Department of Pharmaceutics, Osaka University of Pharmaceutical Sciences, 4–20-1 Nasahara, Takatsuki-city, Osaka 569–1094, Japan

3. Institute of Frontier Medical Sciences, Kyoto University, 53 Kawahara-cho Shogoin, Sakyo-ku, Kyoto 606–8507, Japan

Abstract

Abstract The use of negatively and positively charged gelatin microspheres for pulmonary delivery of salmon calcitonin was examined in rats. The microspheres were prepared using acidic gelatin (isoelectric point (IEP):, 5.0) and basic gelatin (IEP, 9.0) for the negatively and positively charged microspheres, respectively. The average diameters of positively charged gelatin microspheres in the dry state were 3.4, 11.2, 22.5 and 71.5 μm, and that of negatively charged gelatin microspheres was 10.9 μm. Neither positively nor negatively charged gelatin microspheres underwent any degradation in pH 7.0 PBS and there was less than 8% degradation in bronchoalveolar lavage fluid (BALF) after 8 h. In in-vitro release studies in pH 7.0 PBS, salmon calcitonin was rapidly released from positively charged gelatin microspheres within 2 h, and its cumulative release was approximately 85%. In addition, the release profiles were not influenced by particle sizes. The release rates of salmon calcitonin from negatively charged gelatin microspheres were lower than that from positively charged gelatin microspheres. The cumulative release was approximately 40% after 2 h, but there was no evidence of any sustained release. The pulmonary absorption of salmon calcitonin from gelatin microspheres was estimated by measuring its hypocalcaemic effect in rats. The pharmacological availability after administration of salmon calcitonin in positively and negatively charged gelatin microspheres was significantly higher than that in pH 7.0 PBS. The pharmacological availability after administration of salmon calcitonin in positively charged gelatin microspheres was significantly higher than that in negatively charged gelatin microspheres. Administration of salmon calcitonin in positively charged gelatin microspheres with smaller particle sizes led to a higher pharmacological availability. The pharmacological availability after pulmonary administration of salmon calcitonin in positively charged gelatin microspheres with particle sizes of 3.4 and 11.2 μm was approximately 50%. In conclusion, the gelatin microspheres have been shown to be a useful vehicle for pulmonary delivery of salmon calcitonin.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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