Radiopharmacokinetics of Graphene Quantum Dots Nanoparticles In vivo: Comparing the Pharmacokinetics Parameters in Long and Short Periods

Author:

Santos-Oliveira Ralph12,Bastos Matheus Keuper1,Pijeira Martha Sahylí Ortega1,de Souza Sobrinho Juliana Helena3,dos Santos Matos Ana Paula4,Ricci-Junior Eduardo4,de Almeida Fechine Pierre Basilio5,Alencar Luciana Magalhães Rebelo6,Gemini-Piperni Sara7,Alexis Frank8,Attia Mohamed Fathy9

Affiliation:

1. Brazilian Nuclear Energy Commission, Nuclear Engineering Institute, Laboratory of Nanoradiopharmaceuticals and Synthesis of Novel Radiopharmaceuticals, Rio de Janeiro 21941906, Brazil

2. State University of Rio de Janeiro, Laboratory of Radiopharmacy and Nanoradiopharmaceuticals, Rio de Janeiro, 23070200 Brazil

3. Laboratory of Biosystems, Grande Rio University, Rio de Janeiro, 25071-202, Brazil

4. School of Pharmacy, Galenic Development Laboratory (LADEG), Federal University of Rio de Janeiro, Rio de Janeiro, 21941-170, Brazil

5. Group of Chemistry of Advanced Materials (GQMat)- Department of Analytical Chemistry and Physical-Chemistry, Federal University of Ceará, Fortaleza-CE, 451-970, Brazil

6. Department of Physics, Laboratory of Biophysics and Nanosystems, Federal University of Maranhão, Campus Bacanga, São Luís, Maranhão, 65080-805, Brazil

7. Institute of Biological Sciences (ICB), Federal University of Rio de Janeiro, Rio de Janeiro, 21940000 Brazil

8. Politécnico, Quito 170910, Ecuador, Universidad San Francisco de Quito USFQ

9. Center for Nanotechnology in Drug Delivery and Division of Pharmaco-engineering and Molecular Pharmaceutics, Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA

Abstract

Background: Nanoparticles (NPs) have gained great importance during the last decades for developing new therapeutics with improved outcomes for biomedical applications due to their nanoscale size, surface properties, loading capacity, controlled drug release, and distribution. Among the carbon-based nanomaterials, one of the most biocompatible forms of graphene is gra-phene quantum dots (GQDs). GQDs are obtained by converting 2D graphene into zero-dimensional graphene nanosheets. Moreover, very few reports in the literature reported the pharmacokinetic studies proving the safety and effectiveness of GQDs for in vivo applications. Objectives: This study evaluated the pharmacokinetics of GQDs radiolabeled with 99mTc, adminis-tered intravenously, in rodents (Wistar rats) in two conditions: short and long periods, to compare and understand the biological behavior. Methods: The graphene quantum dots were produced and characterized by RX diffractometry, Ra-man spectroscopy, and atomic force microscopy. The pharmacokinetic analysis was performed fol-lowing the radiopharmacokinetics concepts, using radiolabeled graphene quantum dots with techne-tium 99 metastable (99mTc). The radiolabeling process of the graphene quantum dots with 99mTc was performed by the direct via. Results: The results indicate that the pharmacokinetic analyses with GQDs over a longer period were more accurate. Following a bicompartmental model, the long-time analysis considers each pharmacokinetic phase of drugs into the body. Furthermore, the data demonstrated that short-time analysis could lead to distortions in pharmacokinetic parameters, leading to misinterpretations. Conclusion: The evaluation of the pharmacokinetics of GQDs over long periods is more meaning-ful than the evaluation over short periods.

Funder

Carlos Chagas Filho Foundation for Research Support of Rio de Janeiro State

CNPq, Conselho Nacional de Desenvolvimento Científico e Tecnológico

Publisher

Bentham Science Publishers Ltd.

Subject

Drug Discovery,General Medicine

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