1.5-Aminolevulinic acid esters based photodynamic therapy.
Sujuan ZHANG ; Zhenxi ZHANG ; Dazong JIANG
Journal of Biomedical Engineering 2002;19(2):310-314
As exogenous ALA (5-aminolevulinic acid) esters can induce the production and accumulation of endogenous photosensitizer PpIX (protoporphyrin IX) in tumor tissues more effectively, they have been the most active photosensitizer prodrug in PDT(photodynamic therapy) field. In this article, along with the procedure of ALA esters based PDT, some primary mechanism and experimental results were considered, which include: first, cellular uptake of ALA esters and its conversion into ALA; second, the production and accumulation of endogenous photosensitizer PpIX induced by eNdogenous ALA esters; last, the photosensitization of PpIX.
Aminolevulinic Acid
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pharmacology
;
Esters
;
pharmacology
;
Photochemotherapy
;
Photosensitizing Agents
;
pharmacology
;
Prodrugs
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Protoporphyrins
;
pharmacology
2.Preparation of curcumin prodrugs and their in vitro anti-tumor activities.
Peng, LU ; Qiangsong, TONG ; Fengchao, JIANG ; Liduan, ZHENG ; Fangmin, CHEN ; Fuqing, ZENG ; Jihua, DONG ; Yuefeng, DU
Journal of Huazhong University of Science and Technology (Medical Sciences) 2005;25(6):668-70, 678
The curcumin prodrugs, which could be selectively activated in tumor cells, were prepared to establish a basis for the targeted chemotherapy for cancer. On the basis of the molecular structure of curcumin, the N-maleoyl-L-valine-curcumin (NVC), N-maleoyl- glycine-curcumin (NGC) were chemically synthesized and identified by IR and NMR spectroscopy. After treatment with these two prodrugs for 6 - 24 h, the rates of growth inhibition on human bladder cancer EJ cells and renal tubular epithelial (HKC) cells were detected by MTT colorimetry. Our results showed that after the treatment with 20 micromol/L - 40 micromol/L NVC and NGC for 6 - 24 h, the growth inhibitory effects on EJ cells were 6.71% - 65.13% (P < 0.05), 10.96% - 73.01% (P < 0.05), respectively, in both dose- and time-dependent manners. When compared with the curcumin of same concentrations, the growth inhibitory effects of these two prodrugs on HKC cells were significantly decreased (P < 0.01). It is concluded that activation of curcumin prodrugs via hydrolysis functions of cellular esterase could inhibit the growth activities of tumor cells, and reduce the side effects on normal diploid cells. This provided a novel strategy for further exploration of tumor-targeted chemotherapeutic drugs.
Antineoplastic Agents, Phytogenic/*pharmacology
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Curcumin/*pharmacology
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Dose-Response Relationship, Drug
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Prodrugs/*chemical synthesis
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Prodrugs/*pharmacology
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Tumor Cells, Cultured
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Urinary Bladder Neoplasms/*pathology
3.Identification of a new azoreductase driven prodrug from bardoxolone methyl and 5-aminosalicylate for the treatment of colitis in mice.
Xin QIAO ; Yan GONG ; Yi MOU ; Yi-Hua ZHANG ; Zhang-Jian HUANG ; Xiao-Dong WEN
Chinese Journal of Natural Medicines (English Ed.) 2021;19(7):545-550
For local treatment of ulcerative colitis, a new azoreductase driven prodrug CDDO-AZO from bardoxolone methyl (CDDO-Me) and 5-aminosalicylate (5-ASA) was designed, synthesized and biologically evaluated. It is proposed that orally administrated CDDO-AZO is stable before reaching the colon, while it can also be triggered by the presence of azoreductase in the colon to fragment into CDDO-Me and 5-ASA, generating potent anti-colitis effects. Superior to olsalazine (OLS, a clinically used drug for ulcerative colitis) and CDDO-Me plus 5-ASA, CDDO-AZO significantly attenuated inflammatory colitis symptoms in DSS-induced chronic colitis mice, which suggested that CDDO-AZO may be a promising anti-ulcerative colitis agent.
Animals
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Colitis/drug therapy*
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Mesalamine/pharmacology*
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Mice
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Nitroreductases
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Oleanolic Acid/pharmacology*
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Prodrugs
4.Preparation of floxuridine loaded polycation and its antitumor activity.
Dan-Jun ZHAO ; Xiao LU ; Qi-Ying JIANG ; Dan CHEN ; Jun ZHOU ; Hai YU ; Qing-Qing WANG ; Gu-Ping TANG
Journal of Zhejiang University. Medical sciences 2009;38(1):53-58
OBJECTIVETo develop a new prodrug of 5-fluorouracil-polyethylenimine-beta-cyclodextrin-floxuridine (PEI-beta-CyD-Fd) and to test its antitumor activity.
METHODSFloxuridine was conjugated to polyethylenimine-beta-cyclodextrin to form prodrug PEI-beta-CyD-Fd. The structure of synthesized PEI-beta-CyD-Fd was confirmed by (1)H-NMR, FT-IR and UV. MTT assay and cell wound healing assay were performed on human hepatic carcinoma cell line HepG2.
RESULTThe drug loading was 2 %. The MTT assay and cell wound healing assay indicated that PEI-beta-CyD-Fd significantly inhibited proliferation and migration of HepG2 cells.
CONCLUSIONThe synthesized prodrug PEI-CyD-Fd has a significant antitumor activity on HepG2 cells.
Antimetabolites, Antineoplastic ; chemical synthesis ; pharmacology ; Cell Line, Tumor ; Cell Movement ; drug effects ; Cell Proliferation ; drug effects ; Floxuridine ; pharmacology ; Fluorouracil ; pharmacology ; Humans ; Liver Neoplasms ; pathology ; Polyethyleneimine ; pharmacology ; Prodrugs ; chemical synthesis ; pharmacology ; beta-Cyclodextrins ; pharmacology
5.Psammaplin A is a natural prodrug that inhibits class I histone deacetylase.
Dong Hoon KIM ; Jongheon SHIN ; Ho Jeong KWON
Experimental & Molecular Medicine 2007;39(1):47-55
Histone deacetylase (HDAC) has been highlighted as one of key players in tumorigenesis and angiogenesis. Recently, several derivatives of psammaplin (Psams) from a marine sponge have been known to inhibit the HDAC activity, but the molecular mechanism for the inhibition has not fully understood. Here, we explored the mode of action of Psams for the inhibition of HDAC activity in the molecular and cellular level. Among the derivatives, psammaplin A (Psam A) showed the potent inhibitory activity in enzyme assay and anti-proliferation assay with IC50 value of 0.003 and 1 microM, respectively. Psam A selectively induced hyperacetylation of histones in the cells, resulting in the upregulation of gelsolin, a well-known HDAC target gene, in a transcriptional level. In addition, reduced Psam A showed a stronger inhibitory activity than that of non-reduced one. Notably, glutathione-depleted cells were not sensitive to Psam A, implying that cellular reduction of the compound is responsible for the HDAC inhibition of Psam A after uptake into the cells. Together, these data demonstrate that Psam A could exhibit its activity under the reduced condition in the cells and be a new natural prodrug targeting HDAC.
Tyrosine/*analogs & derivatives/chemistry/pharmacology
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Prodrugs/chemistry/*pharmacology
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Oxidation-Reduction
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Molecular Structure
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Humans
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Histones/metabolism
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Histone Deacetylases/*antagonists & inhibitors/*classification/genetics/metabolism
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Hela Cells
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Enzyme Inhibitors/chemistry/*pharmacology
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Disulfides/chemistry/*pharmacology
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Cell Proliferation
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Biological Products/chemistry/*pharmacology
;
Acetylation
6.Recent development of targeted drug delivery system.
Peng-ju ZHOU ; Sheng-qi DENG ; Qian-fei GONG
Acta Pharmaceutica Sinica 2010;45(3):300-306
Targeted drug delivery can significantly increase the concentration of the drug in treatment site, and decrease the dosage of drugs, cost of treatment and the drug's adverse effects on the body. So targeted drug delivery is the hotspot of recent studies. This paper reviews the development of targeted drug delivery research in recent years, including three areas: passive targeting, active targeting, and physical and chemical targeting.
Animals
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Antibodies
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metabolism
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Drug Carriers
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Drug Delivery Systems
;
methods
;
trends
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Emulsions
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Humans
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Liposomes
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Magnetics
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Microspheres
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Nanoparticles
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Pharmaceutical Preparations
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administration & dosage
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Photosensitizing Agents
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pharmacology
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Prodrugs
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Receptors, Cell Surface
;
metabolism
7.Synthesis of precursor of anti-inflammatory agents by using highly reactive zinc.
Aishah AJ ; Nobuhito K ; Tokuda M
The Medical Journal of Malaysia 2004;59 Suppl B():210-211
Highly reactive zinc metal was prepared by electrolysis of a N,N-dimethylformamide (DMF) solution containing naphthalene and a supporting electrolyte in a one-compartment cell fitted with a platinum cathode and a zinc anode. This highly reactive electrogenerated zinc (EGZn/Naph) was used for transformation of ethyl 2-bromoacrylate into the corresponding organozinc compound, which can not be achieved by the use of usual zinc metals. Reaction of the organozinc compounds thus prepared with various aryl halides in the presence of 5 mol% of palladium catalyst gave the corresponding cross-coupling products in high yields. These cross-coupling reactions were successfully applied to a synthesis of the precursor of anti-inflammatory agents such as ibuprofen, naproxen, cicloprofen and suprofen.
Anti-Inflammatory Agents, Non-Steroidal/*chemical synthesis
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Catalysis
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Electrolysis
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Ibuprofen/chemical synthesis
;
Naphthalenes
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Naproxen/chemical synthesis
;
Prodrugs/*chemical synthesis
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Propionic Acids/chemical synthesis
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Suprofen/chemical synthesis
;
Zinc/*pharmacology
8.Design, synthesis and anti-HBV activity of L-amino acid ester prodrugs of acyclic nucleoside phosphonates.
Xiao-Zhong FU ; Sai-Hong JIANG ; Yu-She YANG ; Ru-Yun JI
Acta Pharmaceutica Sinica 2008;43(5):495-503
To design and synthesis a series of novel L-amino acid esters prodrugs of acyclic nucleoside phosphonates with more potent anti-HBV activity, adefovir dipivoxil was used as lead compound, according to the results of enhanced oral bioavailability and antiviral activities of nucleoside L-amino acid ester prodrugs. Eleven novel L-amino acid ester prodrugs of acyclic nucleoside phosphonates were designed and synthesized, their anti-HBV activities were evaluated in HepG2 2.2.15 cells. Eight compounds exhibited antiviral activity, and compound 11 showed the most potent anti-HBV activity and highest selective index in vitro (EC50 0.0952 micromol x L(-1), SI 69523). Moreover, by analyzing the primary structure and activity relationship of these compounds, it could be suggested that L-amino acid ester strategy has significant potential in the acyclic nucleoside phosphonates prodrug design.
Amino Acids
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chemistry
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Antiviral Agents
;
chemical synthesis
;
pharmacology
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Cell Line, Tumor
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Hepatitis B virus
;
drug effects
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Humans
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Liver Neoplasms
;
pathology
;
virology
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Nucleosides
;
chemical synthesis
;
pharmacology
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Organophosphonates
;
chemical synthesis
;
pharmacology
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Prodrugs
;
chemical synthesis
;
pharmacology
9.Synthesis and anticancer activity of norcantharidin-galactose derivatives.
Acta Pharmaceutica Sinica 2008;43(2):157-161
To design and synthesize the hepatic targeting anticancer prodrug with norcantharidin (NCTD-Gal) conjugating structure, galactosylated NCTD derivatives were synthesized from NCTD analogues modified by a series of amino acids via acylation, hydrolysis, glycosylation and deacetylation. Seven new compounds were synthesized as beta-O-glycosides and characterized by IR, MS, NMR and element analysis. The compound 4a was chosen for the inchoate antitumor experiments on mice. The result showed that the antitumor inhibition rate of 4a groups with medium and high dose are clearly higher than that of NCTD group, which suggests that anticancer effect of NCTD is improved at a certain degree by galactosylation.
Animals
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Antineoplastic Agents
;
chemical synthesis
;
pharmacology
;
Bridged Bicyclo Compounds, Heterocyclic
;
chemical synthesis
;
chemistry
;
pharmacology
;
Carcinoma, Hepatocellular
;
pathology
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Cell Line, Tumor
;
Drug Delivery Systems
;
Female
;
Galactose
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chemistry
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Humans
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Liver Neoplasms
;
pathology
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Male
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Mice
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Neoplasm Transplantation
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Prodrugs
;
chemical synthesis
;
pharmacology
10.Synthesis and preliminary evaluation of anti-HIV agent AZT prodrug.
Qing-Bin CUI ; Gao-Xiao ZHANG ; Pei YU ; Yu-Qiang WANG
Acta Pharmaceutica Sinica 2011;46(8):1015-1018
In this research, phosphate and thiophosphate prodrugs 3a, 3b of anti-HIV agent AZT were synthesized, and their anti-HIV activities and cytotoxicities were investigated in vitro. Results showed that the prodrugs 3a and 3b with an IC50 value of 11.0 and 4.0 micromol x L(-1), respectively, were less toxic than AZT (1.0 micromol x L(-1)). Although the EC50 values of both 3a (0.04 micromol x (L(-1) and 3b (0.16 micromol x L(-1)) were lower than that of AZT (0.01 micromol x L(-1)), the therapeutic index (IC50/EC50) of prodrug 3a (275) was much higher than that of both AZT (100) and prodrug 3b (25). This indicated that the prodrug 3a merited further investigation as an anti-HIV agent.
Anti-HIV Agents
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chemical synthesis
;
chemistry
;
pharmacology
;
CD4-Positive T-Lymphocytes
;
cytology
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Cell Proliferation
;
drug effects
;
Cells, Cultured
;
Humans
;
Inhibitory Concentration 50
;
Prodrugs
;
chemical synthesis
;
chemistry
;
pharmacology
;
Zidovudine
;
analogs & derivatives
;
chemical synthesis
;
chemistry
;
pharmacology