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        Extracellular -Glucuronidase for Gene-Directed Enzyme-Prodrug Therapy

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        Most enzymes used for antibody-directed enzyme-prodrug therapy (ADEPT) and gene-directed enzyme-prodrug therapy (GDEPT) are of bacterial, yeast, or viral origin. These xenogeneic proteins can induce an immune response, which might be a hindrance to their application of these enzymes in humans (1 ). On the other hand, when choosing a human enzyme for prodrug conversion cleavage by the respective endogenuous enzyme obviously needs to be avoided. Lysosomal enzymes seem to be particularly suitable candidates, because under normal circumstances, the endogenous enzymes are restricted to intracellular vesicles and therefore not available for premature prodrug conversion. In addition, lysosomal enzymes leaking out of cells are rapidly internalized via the mannose-6-phosphate (M6P) receptor expressed on the surface of most cells and at particulary high levels on reticuloendothelial cells (2 ,3 ). The human lysosomal enzyme β-glucuronidase has been used for ADEPT (4 8 ) and GDEPT (9 ,10 ). This exoglycosidase removes terminal β-glucuronic acids from glycosami-noglycans and other glycoconjugates. The enzyme is highly specific for the glucuronyl residue but has little specificity for the conjugated aglycone. Therefore, different drugs could be developed as prodrugs (see Table 1 ). Elevated β-glucuronidase levels in tumor tissue have been reported, released from dying tumor cells and invading macrophages and neutrophils (18 ,19 ,36 ,37 ). β-Glucuronides of different drugs might be exploited for tumor-specific conversion by released endogenous enzymes (“monotherapy”) as well as for ADEPT and GDEPT approaches.
        Table 1  Glucuronidated Prodrugs Developed for Monotherapy, ADEPT, and GDEPT

        Drug

        Prodrug

        Application

        References

        Anthracyclins

             

        Dpirubicin

        Epirubicin-glucuronide

        ADEPT

        11,12

        Daunorubicin

        Daunorubicin-benzyl carbamate spacer-glucuronide (DNR-GA3)

        Monotherapy, ADEPT

        13–16

        Doxorubicin

        Doxorubicin-benzyl carbamate spacer-glucuronide (Dox-GA3)

        Monotherapy, ADEPT

        7,8,16,17

        Doxorubicin

        Doxorubicin-nitrophenyl spacer-glucuronide (HMR 1826)

        Monotherapy, ADEPT, GDEPT

        5,9,10,18–22

        Daunorubicin and doxorubicin

        Daunorubicin and doxorubicin glucuronides

         

        23

        Doxorubicin

        Doxorubicin-nitrophenyl spacer-glucuronide

         

        24

        Doxorubicin

        Doxorubicin-enol ether spacer-glucuronide

         

        25

        Mustards

             

        Hydroxyaniline mustard (HAM)

        Tetrabutyl HAM glucuronide (BHAMG)

        ADEPT

        26,27

        Mustard

        Mustard-carbamate spacer-glucuronide

         

        28

        Nitrogen mustard

        Nornitrogen mustard-nitrophenyl-glucuronide

         

        29

        Other cytotoxic Drugs

             

        Diverse

        Acetal-glucopyranosiduronates

         

        30

        Rooperol

        Hypoxoside

        Monotherapy

        31

        Palitaxel

        Palitaxel-carbamate-glucuronide

         

        32

        9-Aminocamptothecin

        9-Aminocamptothecin-aromatic spacer-glucuronide

         

        33

        5-Fluorouracil

        5-Fluorouracil-carbamate spacer-glucuronide

        MRS a

        34

        MDR inhibitors

             

        Verapamil, quinine, dipyridamole

        MDR inh. glucuronides (for combination with antracyclin prodrugs)

         

        35

        a MRS, magnetic resonance spectroscopy; MDR inh., multiple drug resistance inhibitors.
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