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WAM Essentials, Inc.
Systemic Enzyme Therapy
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Bromelain proteases suppress growth,
invasion and lung metastasis of B16F10 mouse melanoma cells
1Grabowska E., 1Eckert
K., 2Fichtner I., 1Schulze-Forster
K., and 1Maurer H.R.
1Institut für Pharmazie der Freien Universität
Berlin, 12169 Berlin;
2Max-Delbrück-Centrum für Molekulare
Medizin Berlin-Buch, 13122 Berlin, Germany
International Journal of Oncology 1997, 11, 243-248. |
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Abstract
The thiolprotease bromelain, isolated from pine apple stem,
was suggested for use in adjuvant tumor therapy. This study
examined the in vitro effects of crude bromelain,
bromelain F9 and papain on B16F10 mouse melanoma cell lung
colonization, in vitro cell proliferation, invasion
through matrigel and CD44 expression. In vitro treatment
of the melanoma cells with bromelain F9 and papain before
i.v. injection into mice prevented lung colonization. The
lung weight at day 20 was significantly reduced from 5.1%
(untreated cells) to 1.6% (bromelain F9 treated cells). Papain
was as effective as bromelain F9. However, there was no difference
in the lung weight between bromelain F9 treated and the untreated
group at day 27. Protease removal and further incubation
of the B16F10 cells retained their capacity to induce lung
tumor metastases. The proteases inhibited growth of the melanoma
cells in a dose dependent manner. Crude bromelain was most
active with a half maximal value of 7.5 mg/ml. However, the
antiproliferative effects did not correlate with the proteolytic
activity. In a matrigel invasion assay, the proteases reduced
the invasive capacity of the melanoma cells maximally by
about 30%. Using flow cytometry, the proteases were found
to reduce the CD44 intensity, present on the melanoma cells,
to a different degree: crude bromelain was more active than
bromelain F9 and papain, which had higher proteolytic activity.
Crude bromelain was most active in abolishing the CD44 re-expression
after protease treatment.
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