Fabrication of microcapsules with core‐shell structure for oral delivery of dual drugs and real‐time computed tomography imaging

Although multidrug combinations are an effective therapeutic strategy for serious disease in clinical practice, their therapeutic effect may be reduced because they conflict with each other medicinally in certain cases. Hence, there is an urgent need to develop a single drug carrier for precise mult...

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Published inIET nanobiotechnology Vol. 15; no. 7; pp. 619 - 626
Main Authors Cai, Rong, Xiao, Long, Zhang, Miaomiao, Zhao, Lulu, Zhang, Jingjing, Du, Fengyi, Wang, Zhirong
Format Journal Article
LanguageEnglish
Published United States John Wiley & Sons, Inc 01.09.2021
John Wiley and Sons Inc
Wiley
Subjects
Administration, Oral
Barium
Barium sulfate
biomedical materials
cancer
Capsules
cellular biophysics
computerised tomography
CT imaging
Diagnostic imaging
diseases
Drug Carriers
Drug delivery systems
Drugs
Health aspects
Original Research Paper
Original Research Papers
Particle Size
Real-time control
Real-time systems
Tomography, X-Ray Computed
Vehicles
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Summary:Although multidrug combinations are an effective therapeutic strategy for serious disease in clinical practice, their therapeutic effect may be reduced because they conflict with each other medicinally in certain cases. Hence, there is an urgent need to develop a single drug carrier for precise multidrug delivery to avoid this interference. A reverse coordination method is reported that fabricates a double‐layer barium sulphate microcapsule (DL@BS MS) for two drugs separately loading simultaneously. In addition, BS nanoclusters were synthesised in situ inside the DL@BS MSs for real‐time computed tomography (CT) imaging. The results showed that the DL@BS MSs with a particle size of approximately 2 mm exhibited a uniform sphere. Because BS nanoclusters have a high X‐ray attenuation coefficient, the retention of DL@BS MSs in the digestive tract could be monitored through CT imaging in real time. More important, the core‐shell structure of DL@BS MSs encapsulating two different drugs could be released in spatiotemporal order in an acidic stomach environment. The as‐synthesis DL@BS MSs with a core‐shell structure and real‐time imaging performance provide an ideal carrier for the oral administration of multiple drugs simultaneously loaded but sequentially released.
Bibliography:Rong Cai and Long Xiao have contributed equally to this work.
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ISSN:1751-8741
1751-875X
DOI:10.1049/nbt2.12058