Design and Characterizations of Inhalable Poly(lactic-co-glycolic acid) Microspheres Prepared by the Fine Droplet Drying Process for a Sustained Effect of Salmon Calcitonin

Sato, Hideyuki; Tabata, Aiko; Moritani, Tatsuru; Morinaga, Tadahiko; Mizumoto, Takao; Seto, Yoshiki; Onoue, Satomi

doi:10.3390/molecules25061311

Cited by 14 publications

(9 citation statements)

References 44 publications

(52 reference statements)

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“…Our observation of relatively higher affinity of sCT compared to hCT towards calcitonin receptor and its signalling is consistent with previous reports. 2,5,13 In contrast to the general assumption of higher binding of calcitonin to albumin in plasma, 2,5,13 we observed that both hCT and sCT had weaker affinity to albumin compared to its affinity to other plasma proteins. In the plasma both hCT and sCT were observed to have superior affinity to beta-2-microglobulin's, although the physiological significance of this is unknown.…”

Section: Discussioncontrasting

confidence: 78%

“…12 Several attempts are also being made to enhance the pharmacokinetics of CT to further increase its bioavailability and achieve sustained delivery. 13,14 The sustained pharmacodynamic effects of CT despite the limitations with its pharmacokinetics calls to question if such attempts to further improve the pharmacokinetics of CT are necessary especially when this can lead to several undesirable pharmacodynamic and adverse effects. Further the variability observed between the pharmacokinetics vs pharmacodynamic effects of CT may paraphs indicate a unique compartmentalization of CT in the blood.…”

Section: Introductionmentioning

confidence: 99%

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Protein Binding and Differential Distribution of Calcitonin in the Sub-compartments of Blood: An in vitro Study

Bryan

Kumar

2022

BEMS Reports

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The pharmacodynamics effects of therapeutically administered calcitonin is observed for extended duration much beyond its reported short half-life. The rationale for this pharmacodynamic-pharmacokinetics mismatch of calcitonin is not known. Hence in this study the hypothesis on sub-compartmentalization of calcitonin in blood to explain the extended pharmacodynamics effects of calcitonin was evaluated in vitro using the sheep blood model. A relatively higher proportion of calcitonin concentration was observed in the WBC compartment. The partition coefficient analysis showed levels of calcitonin to be higher on WBC membrane compared to intracellular. Molecular modelling to assess the binding of calcitonin with protein in plasma and WBC membranes indicated physiologically relevant higher affinity with beta-2-microglobulin's in plasma and glycoproteins (CD44), sushi domains (CD25), fibronectins (CD206) and siglecs (CD22) on WBC membrane. The physiologically relevant higher affinity with several proteins on WBC membrane and plasma can be responsible for extended pharmacodynamics effects observed for therapeutically administered calcitonin.

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Section: Discussioncontrasting

confidence: 78%

Section: Introductionmentioning

confidence: 99%

Protein Binding and Differential Distribution of Calcitonin in the Sub-compartments of Blood: An in vitro Study

Bryan

Kumar

2022

BEMS Reports

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“…Another category of strategies for efficient, improved, and long-acting administration of peptides is based on the encapsulation and delivery of peptides using advanced formulations and materials such as micro/nanoparticles, − hydrogels, − particle/hydrogel composites, , polymeric and naturally derived scaffolds, − and stimuli-responsive materials − (Figure ). Such platforms are anticipated to overcome major hurdles that therapeutic peptide delivery has been encountered and illustrate great potential for sustained and controlled delivery of peptides .…”

Section: Strategies To Tackle the Limitations Of Therapeutic Peptide ...mentioning

confidence: 99%

Recent Advances in Formulations for Long-Acting Delivery of Therapeutic Peptides

Zangabad

Rezvani

Tong

et al. 2023

ACS Appl. Bio Mater.

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Recent preclinical and clinical studies have focused on the active area of therapeutic peptides due to their high potency, selectivity, and specificity in treating a broad range of diseases. However, therapeutic peptides suffer from multiple disadvantages, such as limited oral bioavailability, short half-life, rapid clearance from the body, and susceptibility to physiological conditions (e.g., acidic pH and enzymolysis). Therefore, high peptide dosages and dose frequencies are required for effective patient treatment. Recent innovations in pharmaceutical formulations have substantially improved therapeutic peptide administration by providing the following advantages: long-acting delivery, precise dose administration, retention of biological activity, and improvement of patient compliance. This review discusses therapeutic peptides and challenges in their delivery and explores recent peptide delivery formulations, including micro/nanoparticles (based on lipids, polymers, porous silicon, silica, and stimuli-responsive materials), (stimuli-responsive) hydrogels, particle/hydrogel composites, and (natural or synthetic) scaffolds. This review further covers the applications of these formulations for prolonged delivery and sustained release of therapeutic peptides and their impact on peptide bioactivity, loading efficiency, and (in vitro/in vivo) release parameters.

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“…Concerning the administration of biologics, parenteral routes, such as intravenous and/or intramuscular injections, have been mostly used due to their low oral bioavailability and stability in the gastrointestinal tract, which can negatively affect patient compliance. As an alternative non-invasive route for the administration of pharmaceutical ingredients, recently pharmaceutical researchers have focused their studies on pulmonary delivery [76]. The pulmonary route is an attractive target for both local and systemic drug delivery due to benefits, such as rich blood supply, large surface area, and absence of firstpass metabolism.…”

Section: Plga Microparticlesmentioning

confidence: 99%

Poly(Lactic Acid)-Based Microparticles for Drug Delivery Applications: An Overview of Recent Advances

et al. 2022

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The sustained release of pharmaceutical substances remains the most convenient way of drug delivery. Hence, a great variety of reports can be traced in the open literature associated with drug delivery systems (DDS). Specifically, the use of microparticle systems has received special attention during the past two decades. Polymeric microparticles (MPs) are acknowledged as very prevalent carriers toward an enhanced bio-distribution and bioavailability of both hydrophilic and lipophilic drug substances. Poly(lactic acid) (PLA), poly(lactic-co-glycolic acid) (PLGA), and their copolymers are among the most frequently used biodegradable polymers for encapsulated drugs. This review describes the current state-of-the-art research in the study of poly(lactic acid)/poly(lactic-co-glycolic acid) microparticles and PLA-copolymers with other aliphatic acids as drug delivery devices for increasing the efficiency of drug delivery, enhancing the release profile, and drug targeting of active pharmaceutical ingredients (API). Potential advances in generics and the constant discovery of therapeutic peptides will hopefully promote the success of microsphere technology.

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Design and Characterizations of Inhalable Poly(lactic-co-glycolic acid) Microspheres Prepared by the Fine Droplet Drying Process for a Sustained Effect of Salmon Calcitonin

Cited by 14 publications

References 44 publications

Protein Binding and Differential Distribution of Calcitonin in the Sub-compartments of Blood: An in vitro Study

Protein Binding and Differential Distribution of Calcitonin in the Sub-compartments of Blood: An in vitro Study

Recent Advances in Formulations for Long-Acting Delivery of Therapeutic Peptides

Poly(Lactic Acid)-Based Microparticles for Drug Delivery Applications: An Overview of Recent Advances

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