GET THE APP

Biomedical Applications of Nanoparticles
..

Epilepsy Journal

ISSN: 2472-0895

Open Access

Editorial - (2022) Volume 8, Issue 2

Biomedical Applications of Nanoparticles

Manik Prabhu*
*Correspondence: Manik Prabhu, Department of Pharmacy, Osmania University, Hyderabad, Telangana, India, Email:
Department of Pharmacy, Osmania University, Hyderabad, Telangana, India

Received: 05-Mar-2022, Manuscript No. elj-22-59482; Editor assigned: 07-Mar-2022, Pre QC No. P-59482; Reviewed: 18-Mar-2022, QC No. Q-59482; Revised: 25-Mar-2022, Manuscript No. R-59482; Published: 31-Mar-2022 , DOI: 10.37421/elj.2022.8.159
Citation: Prabhu, Manik. “Biomedical Applications of Nanoparticles.” Epilepsy J 8 (2022): 159. DOI: 10.37421/elj.2022.8.159
Copyright: © 2022 Prabhu M. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Editorial

For the treatment of brain illnesses, nanotechnology has opened up a whole new universe of possibilities. Nanosystems can encapsulate, transport, and administer a wide range of therapeutic substances, including medicines and nucleic acids. Nanoparticles can also be manufactured to include photosensitizers or act as photothermal conversion agents in phototherapy on their own. Nano-delivery agents can also improve the efficacy of contrast agents, allowing for better brain imaging and diagnosis. The blood–brain barrier, on the other hand, makes effective nano-delivery to the brain difficult (BBB). Advances in understanding natural transport channels through the BBB have led to the possibility of using receptor-mediated transcytosis as a method of nanoparticle absorption. As a targeted ligand, the oligopeptide Angiopep-2, which has a high BBB transcytosis potential, has been used. Angiopep-2 has been functionalized on a variety of organic and inorganic nanostructures to route medicinal and diagnostic substances to the brain. These have showed considerable promise not just in the treatment and diagnosis of brain cancer, but also in the treatment of brain damage, stroke, epilepsy, Parkinson's disease, and Alzheimer's disease. This review focuses on studies using Angiopep-2-modified nanoparticles for the treatment and diagnostics of brain diseases done between 2010 and 2021 [1].

"BBB-crossing nanotechnology is predicted to have a transformative influence on traditional brain cancer management," Tang and colleagues. Angiopep-2-mediated transport techniques are becoming increasingly significant in this area. Most Angiopep-2-functionalized nanomedicines are currently being used to treat brain tumours, particularly glioblastoma, which is very aggressive and resistant to current treatment.

Angiopep-2 alteration has the advantage of being able to penetrate both the BBB and the blood-tumor barrier (BTB). There is minimal comparative data on the performance of Angiopep-2 vs. other cell-penetrating peptides that we are aware of. Co-modification of NP with Angiopep-2 and other cell-penetrating peptides has been demonstrated to improve NP function. Functionalization of the chemotherapeutic drug PAPTP with either Angiopep-2 or the TAT48-61 peptide, on the other hand, allowed equivalent transport to the brain in mice [2].

The as-functionalized nanosystems have also shown promise in the delivery of drugs to treat other brain illnesses, such as fungal infections, epilepsy, stroke, brain injury, Parkinson's disease, and Alzheimer's disease, in the last five years. In a Caenorhabditis elegans model of Alzheimer's disease, gold nanorods functionalized with Angiopep-2 and the D1 peptide, which identifies hazardous clumps of -amyloid, exhibited effectiveness [3].

Angiopep-2-decorated nanostructures have been used to deliver a wide range of medicinal and diagnostic substances within the time period evaluated for this review. Chemical substances, nucleic acids such as DNA, siRNA, and miRNA, photosensitizers, and contrast agents are among them. Angiopep-2-modified nanoparticles can also be used in immunotherapy. Angiopep-2 and IP10-EGFRvIIIscFv fusion protein-modified NPs can recruit activated CD8+ T lymphocytes to glioblastoma cells, according to Wang and colleagues [4].

While the use of Angiopep-2-modified NPs in phototherapy is well known, Sonodynamic Therapy (SDT), a unique physical technique of eliminating brain cancer cells based on ultrasound stimulation, has recently been published. Qu and his colleagues created "all-in-one" nanosensitizer platform by combining the sonoactive chlorin e6 and an autophagy inhibitor, hydroxychloroquine, in Angiopep-2-modified liposomes to promote apoptosis and inhibit mitophagy with glioma cells at the same time [1,3].

Angiopep-2 NPs, like those in the previous study, are responsive to dual- and multimodal treatment integration. Angiopep-2 nanosystems can also be made to respond to stimuli in order to deliver their therapeutic cargo in a regulated and continuous manner. Furthermore, their potential in theranostics has recently been recognised. There is a growing corpus of in vivo data to support the development of multifunctional Angiopep-2-modified nanomedicines, which is encouraging. Overall, there is a pressing need to bring BBB-crossing nanotherapeutics' in vitro and in vivo successes to the clinic [5].

Conflict of Interest

None.

Acknowledgement

None.

References

  1. Bellettato, M Cinzia, and Scarpa Maurizio. “Possible strategies to cross the blood–brain barrier.” Ital J Pediatr, 44(2018):127-133.
  2. Google Scholar, Crossref

  3. O’Keeffe, Eoin, and Campbell Matthew. “Modulating the paracellular pathway at the blood–brain barrier: Current and future approaches for drug delivery to the CNS.” Drug Discov Today Technol, 20(2016):35-39.
  4. Google Scholar, Crossref

  5. Ceña, Valentín, and Játiva Pablo. “Nanoparticle crossing of blood-brain barrier: A road to new therapeutic approaches to central nervous system diseases.” Future Med, 13(2018):1513-1516.
  6. Google Scholar, Crossref

  7. Demeule, Michel, Regina Anthony, Che Christian, and Poirier Julie, et al. “Identification and design of peptides as a new drug delivery system for the brain.” J Pharmacol Exp Ther, 324(2008):1064-1072.
  8. Google Scholar, Crossref

  9. Regina, A, Demeule M, Che C, and Lavallee I, et al. “Antitumour activity of ANG1005, a conjugate between paclitaxel and the new brain delivery vector Angiopep-2.” Br J Pharmacol, 155(2008):185-197.
  10. Google Scholar, Crossref

arrow_upward arrow_upward