Preparation of AHTG-DNR conjugates and their antitumor effect in vitro

Zhang Dong-hua; Tang Jin-zhi; Shen Guan-xin; Shu Na; Zhu Hui-fen

doi:10.1007/BF02887937

Current Medical Science ›› 1990, Vol. 10 ›› Issue (4) DOI: 10.1007/BF02887937

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Preparation of AHTG-DNR conjugates and their antitumor effect in vitro

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Abstract

100%, 75%, 50%, 25% and 12.5% oxidized dextran T10 (Dex T1o) were used as intermediate carriers for conjugating drug daunorubicin (DNR) and antibody anti-human thymocitic globulin (AHTG), to form different immunoconjugates, AHTG:Dex:DNR. It was demonstrated that the conjugate with 25% oxidized Dex T10 as intermediate carrier linked more DNR molecules than the others. The degree of its substitution was 10–11 moles of DNR per mole of AHTG. Moreover, because the amount to reducing agent sodium borohydride (NaBH₄), required for the reduction reaction, was relatively small, its damaging effect on AHTG and DNR was lessened accordingly.

The antitumor effect of AHTG: Dex: DNR in vitro was tested by using 24-h cytotoxicity assay, with CEM as target cell. Cytotoxic effect of the conjugate was proven and the LD₅₆ was 10.68 μg/ml. However, it showed only slight cytotoxic effect on non-target cell K562. When 10 min cytotoxicity assay was performed to show the specific tumor-killing effect of the conjugate, it revealed an obvious cytotoxic activity toward CEM, with the LD₅₀ being 14.79 μg/ml, but hardly toward K562. These results suggest that AHTG:Dex:DNR possesses specific cytotoxic effect.

Keywords

immunoconjugate / AHTG / daunorubicin / cell lines

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Zhang Dong-hua, Tang Jin-zhi, Shen Guan-xin, Shu Na, Zhu Hui-fen. Preparation of AHTG-DNR conjugates and their antitumor effect in vitro. Current Medical Science, 1990, 10(4): DOI:10.1007/BF02887937

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References

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[1]	HurwitzE, et al.. Site-directed chemotherapy with a drug bound to anti-idiotypic antibody to a lymphoma cellsurface IgM. Int J Cancer, 1983, 31: 745-8

[2]	TsukadaY, et al.. An anti-α-fetoprotein antibody-daunorubicin conjugate with a novel poly-L-glutamic acid derivative as intermediate drug carrier. J Natl Cancer Inst, 1984, 73: 721-9

[3]	BernstainA, et al.. Higher antitumor efficacy of daunomycin when linked to dextran: in vivo and in vitro studies. J Natl Cancer Inst, 1978, 60: 379-84

[4]	HurwitzE, et al.. The covalent binding of daunomycin and adriamycin to antibodies, with retention of both drug and antibody activities. Cancer Res, 1975, 35: 1175-81

[5]	HurwitzE, et al.. The effect in vivo of chemotherapeutic drug-antibody conjugates in two murine experimental tumor systems. Int J Cancer, 1978, 21: 745-55

[6]	ArnonR, SelaM. In vitro and in vivo efficacy of conjugates of daunomycin with anti-tumor antibodies. Immunological Res, 1982, 62: 5-27

[7]	GhoseTI, et al.. Preparation of antibodylinked cytotoxic agents. Methods Enzymol, 1983, 93: 280-333

[8]	GallegoJ, et al.. Preparation of four daunomycin-monoclonal antibody 791 T/ 36 conjugates with anti-tumor activity. Int J Cancer, 1984, 33: 737-44

[9]	LevyR, et al.. The specific cytotoxic effects of daunomycin conjugated to antitumor antibodies. Cancer Res, 1975, 35: 1182-6

[10]

1981

[11]	DeguchiT, et al.. Potential therapeutic effects of adriamycin-monoclonal anti-prostatic acid phosphatase antibody conjugate on human p rostate tumor. J Urol, 1987, 137: 353-8