SAINS MALAYSIANA

Sains Malaysiana 50(12)(2021): 3693-3703

http://doi.org/10.17576/jsm-2021-5012-19

A Brief Review on Hydrophobic Modifications of Glycol Chitosan into Amphiphilic Nanoparticles for Enhanced Drug Delivery

(Suatu Ulasan Ringkas pada Pengubahsuaian Hidrofobi Glikol Kitosan kepada Zarah Nano Amfifili untuk Penambahbaikan Penghantaran Dadah)

WAI MUN CHONG¹ & ERAZULIANA ABD KADIR¹*

¹Integrative Medicine Cluster, Advanced Medical and Dental Institute, Universiti Sains Malaysia, Bertam, 13200 Kepala Batas, Pulau Pinang, Malaysia

Diserahkan: 16 Mac 2021/Diterima: 9 April 2021

ABSTRACT

Glycol chitosan (GC) is the chitosan derivative that is capable of forming amphiphilic nanoparticles upon structure modifications at the reactive functional amine group on the polymer sugar backbone. Owing to the hydrophilic feature of GC and hydrophobic moieties that can be added to the GC structure, modifiable nanosystems were constructed to entrap poorly soluble drugs, mostly chemotherapeutic agents and several anti-inflammatory, anaesthetic, immunosuppressant, and antifungal drugs for more efficient delivery of the payload to the target site and improving the intended therapeutic effects. This review highlights the various hydrophobic molecules used in the chemical modification of GC to create amphiphilic nanoparticles for hydrophobic drug delivery, along with the summary of their physicochemical criteria and successful therapeutic enhancement achieved with the application of the drug-loaded amphiphiles. The biodegradable, GC-based nanoparticles particularly having the inner hydrophobic core and outer hydrophilic shell are an efficient system for drug entrapment, protection and targeting to improve the bioavailability and safety of the drug, in particular for cancer treatment purposes. The significant drug delivery enhancements achieved by these various hydrophobically-modified GC nanoparticles may provide the insights for their further use in nanomedicine.

Keywords: Amphiphiles; drug delivery; glycol chitosan; hydrophobic drugs; nanoparticles

ABSTRAK

Glikol kitosan (GC) adalah bahan terbitan kitosan yang berupaya membentuk zarah nano amfifili dengan pengubahsuaian struktur kumpulan amina berfungsian reaktif pada tulang belakang gula polimer. Disebabkan sifat hidrofili GC dan moieti hidrofobi yang boleh ditambah pada struktur GC, nanosistem boleh ubah suai telah dicipta untuk memerangkap dadah kurang larut, kebanyakannya agen kemoterapi dan beberapa dadah antiradang, anestetik, imunosupresan dan antikulat untuk penghantaran bahan muatan tersebut ke tempat sasaran dengan lebih berkesan dan menambah baik kesan terapeutik yang dikehendaki. Ulasan ini menekankan pelbagai molekul hidrofobi yang digunakan dalam pengubahsuaian kimia pada GC untuk mencipta zarah nano amfifili dalam penghantaran dadah hidrofobi, berserta ringkasan kriteria fizikokimia dan penambahbaikan terapeutik yang berjaya dicapai dengan aplikasi amfifil berisikan dadah. Amfifil terbiodegradasikan berasaskan GC ini membentuk zarah nano secara khususnya mempunyai teras hidrofobi dan cangkerang hidrofili untuk pemerangkapan, perlindungan dan penyasaran dadah untuk menambah baik ketersediaan bio dan keselamatan dadah tersebut, secara khususnya untuk tujuan rawatan kanser. Penambahbaikan ketara dalam penghantaran dadah yang dicapai oleh pelbagai pengubahsuaian hidrofobi pada zarah nano GC ini mungkin dapat memberikan satu wawasan untuk penggunaannya yang lebih mendalam dalam bidang nanoperubatan.

Kata kunci: Amfifil; dadah hidrofobi; glikol kitosan; penghantaran dadah; zarah nano

RUJUKAN

Ahmad, S., Johnston, B.F., Mackay, S.P., Schatzlein, A.G., Gellert, P., Sengupta, D. & Uchegbu, I.F. 2010. In silico modelling of drug-polymer interactions for pharmaceutical formulations. Journal of the Royal Society Interface 7(4): S423-S433.

Amreddy, N., Babu, A., Muralidharan, R., Panneerselvam, J., Srivastava, A., Ahmed, R., Mehta, M., Munshi, A. & Ramesh, R. 2018. Recent advances in nanoparticle-based cancer drug and gene delivery. Advances in Cancer Research 137: 115-170.

Choi, Y., Lim, S., Yoon, H.Y., Kim, B.S., Kwon, I.C. & Kim, K. 2019. Tumor-targeting glycol chitosan nanocarriers: Overcoming the challenges posed by chemotherapeutics. Expert Opinion on Drug Delivery 16(8): 835-846.

Chooi, K.W., Carlos, M.I.S., Soundararajan, R., Gaisford, S., Arifin, N., Schätzlein, A.G. & Uchegbu, I.F. 2014. Physical characterisation and long-term stability studies on quaternary ammonium palmitoyl glycol chitosan (GCPQ) - A new drug delivery polymer. Journal of Pharmaceutical Sciences 103(8): 2296-2306.

Duhem, N., Rolland, J., Riva, R., Guillet, P., Schumers, J.M., Jérome, C., Gohy, J.F. & Préat, V. 2012. Tocol modified glycol chitosan for the oral delivery of poorly soluble drugs. International Journal of Pharmaceutics 423(2): 452-460.

Feng, X., Zhou, Y., Xie, X., Li, M., Huang, H., Wang, L., Xu, X. & Yu, J. 2019. Development of PSMA-targeted and core-crosslinked glycol chitosan micelles for docetaxel delivery in prostate cancer therapy. Materials Science and Engineering: C 96: 436-445.

Fisusi, F.A., Siew, A., Chooi, K.W., Okubanjo, O., Garrett, N., Lalatsa, K., Serrano, D., Summers, I., Moger, J., Stapleton, P. & Satchi-Fainaro, R. 2016. Lomustine nanoparticles enable both bone marrow sparing and high brain drug levels - A strategy for brain cancer treatments. Pharmaceutical Research 33(5): 1289-1303.

Ghaz-Jahanian, M.A., Abbaspour-Aghdam, F., Anarjan, N., Berenjian, A. & Jafarizadeh-Malmiri, H. 2015. Application of chitosan-based nanocarriers in tumor-targeted drug delivery. Molecular Biotechnology 57(3): 201-218.

Hwang, H.Y., Kim, I.S., Kwon, I.C. & Kim, Y.H. 2008. Tumor targetability and antitumor effect of docetaxel-loaded hydrophobically modified glycol chitosan nanoparticles. Journal of Controlled Release 128(1): 23-31.

Kanwal, U., Bukhari, N.I., Rana, N.F., Rehman, M., Hussain, K., Abbas, N., Mehmood, A. & Raza, A. 2019. Doxorubicin-loaded quaternary ammonium palmitoyl glycol chitosan polymeric nanoformulation: Uptake by cells and organs. International Journal of Nanomedicine 14: 1-15.

Karlsson, J., Vaughan, H.J. & Green, J.J. 2018. Biodegradable polymeric nanoparticles for therapeutic cancer treatments. Annual Review of Chemical and Biomolecular Engineering 9: 105-127.

Kim, J.H., Kim, Y.S., Park, K., Lee, S., Nam, H.Y., Min, K.H., Jo, H.G., Park, J.H., Choi, K., Jeong, S.Y. & Park, R.W. 2008. Antitumor efficacy of cisplatin-loaded glycol chitosan nanoparticles in tumor-bearing mice. Journal of Controlled Release 127(1): 41-49.

Kim, J.H., Kim, Y.S., Kim, S., Park, J.H., Kim, K., Choi, K., Chung, H., Jeong, S.Y., Park, R.W., Kim, I.S. & Kwon, I.C. 2006. Hydrophobically modified glycol chitosan nanoparticles as carriers for paclitaxel. Journal of Controlled Release 111(1-2): 228-234.

Kim, K., Kim, J.H., Park, H., Kim, Y.S., Park, K., Nam, H., Lee, S., Park, J.H., Park, R.W., Kim, I.S. & Choi, K. 2010. Tumor-homing multifunctional nanoparticles for cancer theragnosis: Simultaneous diagnosis, drug delivery, and therapeutic monitoring. Journal of Controlled Release 146(2): 219-227.

Kim, S.E., Kim, H.J., Rhee, J.K. & Park, K. 2017. Versatile chemical derivatizations to design glycol chitosan-based drug carriers. Molecules 22(10): 662.

Koo, H., Min, K.H., Lee, S.C., Park, J.H., Park, K., Jeong, S.Y., Choi, K., Kwon, I.C. & Kim, K. 2013. Enhanced drug-loading and therapeutic efficacy of hydrotropic oligomer-conjugated glycol chitosan nanoparticles for tumor-targeted paclitaxel delivery. Journal of Controlled Release 172(3): 823-831.

Kwon, S., Park, J.H., Chung, H., Kwon, I.C., Jeong, S.Y. & Kim, I.S. 2003. Physicochemical characteristics of self-assembled nanoparticles based on glycol chitosan bearing 5β-cholanic acid. Langmuir 19(24): 10188-10193.

Lee, B.S., Park, K., Park, S., Kim, G.C., Kim, H.J., Lee, S., Kil, H., Oh, S.J., Chi, D., Kim, K. & Choi, K. 2010. Tumor targeting efficiency of bare nanoparticles does not mean the efficacy of loaded anticancer drugs: Importance of radionuclide imaging for optimization of highly selective tumor targeting polymeric nanoparticles with or without drug. Journal of Controlled Release 147(2): 253-260.

Loftsson, T. & Brewster, M.E. 2010. Pharmaceutical applications of cyclodextrins: Basic science and product development. Journal of Pharmacy and Pharmacology 62(11): 1607-1621.

Meng, L., Huang, W., Wang, D., Huang, X., Zhu, X. & Yan, D. 2013. Chitosan-based nanocarriers with pH and light dual response for anticancer drug delivery. Biomacromolecules 14(8): 2601-2610.

Mennini, N., Furlanetto, S., Bragagni, M., Ghelardini, C., Di Cesare Mannelli, L. & Mura, P. 2014. Development of a chitosan-derivative micellar formulation to improve celecoxib solubility and bioavailability. Drug Development and Industrial Pharmacy 40(11): 1494-1502.

Min, K.H., Park, K., Kim, Y.S., Bae, S.M., Lee, S., Jo, H.G., Park, R.W., Kim, I.S., Jeong, S.Y., Kim, K. & Kwon, I.C. 2008. Hydrophobically modified glycol chitosan nanoparticles-encapsulated camptothecin enhance the drug stability and tumor targeting in cancer therapy. Journal of Controlled Release 127(3): 208-218.

Nair, L.S. & Laurencin, C.T. 2007. Biodegradable polymers as biomaterials. Progress in Polymer Science 2(8-9): 762-798.

Park, J.S., Han, T.H., Lee, K.Y., Han, S.S., Hwang, J.J., Moon, D.H., Kim, S.Y. & Cho, Y.W. 2006. N-acetyl histidine-conjugated glycol chitosan self-assembled nanoparticles for intracytoplasmic delivery of drugs: Endocytosis, exocytosis and drug release. Journal of Controlled Release 115(1): 37-45.

Qu, X., Khutoryanskiy, V.V., Stewart, A., Rahman, S., Papahadjopoulos-Sternberg, B., Dufes, C., McCarthy, D., Wilson, C.G., Lyons, R., Carter, K.C. & Schätzlein, A. 2006. Carbohydrate-based micelle clusters which enhance hydrophobic drug bioavailability by up to 1 order of magnitude. Biomacromolecules 7(12): 3452-3459.

Razi, M.A., Wakabayashi, R., Goto, M. & Kamiya, N. 2019. Self-assembled reduced albumin and glycol chitosan nanoparticles for paclitaxel delivery. Langmuir 35(7): 2610-2618.

Saravanakumar, G., Min, K.H., Min, D.S., Kim, A.Y., Lee, C.M., Cho, Y.W., Lee, S.C., Kim, K., Jeong, S.Y., Park, K. & Park, J.H. 2009. Hydrotropic oligomer-conjugated glycol chitosan as a carrier of paclitaxel: Synthesis, characterization, and in vivo biodistribution. Journal of Controlled Release 140(3): 210-217.

Siew, A., Le, H., Thiovolet, M., Gellert, P., Schatzlein, A. & Uchegbu, I. 2012. Enhanced oral absorption of hydrophobic and hydrophilic drugs using quaternary ammonium palmitoyl glycol chitosan nanoparticles. Molecular Pharmaceutics 9(1): 14-28.

Trapani, A., Sitterberg, J., Bakowsky, U. & Kissel, T. 2009. The potential of glycol chitosan nanoparticles as carrier for low water soluble drugs. International Journal of Pharmaceutics 375(1-2): 97-106.

Uchegbu, I.F., Sadiq, L., Arastoo, M., Gray, A.I., Wang, W., Waigh, R.D. & Schätzleinä, A.G. 2001. Quaternary ammonium palmitoyl glycol chitosan - A new polysoap for drug delivery. International Journal of Pharmaceutics 224(1-2): 185-199.

Vivek, R., Babu, V.N., Thangam, R., Subramanian, K.S. & Kannan, S. 2013. pH-responsive drug delivery of chitosan nanoparticles as Tamoxifen carriers for effective anti-tumor activity in breast cancer cells. Colloids and Surfaces B: Biointerfaces 111: 117-123.

Wang, J.J., Zeng, Z.W., Xiao, R.Z., Xie, T., Zhou, G.L., Zhan, X.R. & Wang, S.L. 2011. Recent advances of chitosan nanoparticles as drug carriers. International Journal of Nanomedicine 6: 765.

Xu, J., Yu, J., Xu, X., Wang, L., Liu, Y., Li, L., Zhao, J. & He, M. 2014. Development, characterization, and evaluation of PSMA-targeted glycol chitosan micelles for prostate cancer therapy. Journal of Nanomaterials 2014: Article ID. 462356.

Yang, H., Tang, C. & Yin, C. 2018. Estrone-modified pH-sensitive glycol chitosan nanoparticles for drug delivery in breast cancer. Acta Biomaterialia 73: 400-411.

Yu, J.M., Li, Y.J., Qiu, L.Y. & Jin, Y. 2009. Polymeric nanoparticles of cholesterol-modified glycol chitosan for doxorubicin delivery: Preparation and in-vitro and in-vivo characterization. Journal of Pharmacy and Pharmacology 61(6): 713-719.

Yu, J.M., Li, Y.J., Qiu, L.Y. & Jin, Y. 2008. Self-aggregated nanoparticles of cholesterol-modified glycol chitosan conjugate: Preparation, characterization, and preliminary assessment as a new drug delivery carrier. European Polymer Journal 44(3): 555-565.

Zhou, Y., Yu, J., Feng, X., Li, W., Wang, Y., Jin, H., Huang, H., Liu, Y. & Fan, D. 2016. Reduction-responsive core-crosslinked micelles based on a glycol chitosan-lipoic acid conjugate for triggered release of doxorubicin. RSC Advances 6(37): 31391-31400.

*Pengarang untuk surat-menyurat; email: erazuliana@usm.my

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