Terbinafine 抑制人類上皮癌細胞﹙ A431﹚ 生長機制之研究

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Terbinafine

抑制人類上皮癌細胞﹙ A431﹚ 生長機制之研究

 Terbinafine (TB) 是一種被廣泛使用的抗黴菌藥物，經過實驗已經證實對人類大腸癌細胞 Colo 205 可促使其細胞週期停滯於 G0/G1 期而抑制其生長。在本實驗中則主要研究 TB 對人類上皮癌細胞 (A431) 的作用機制。首先，在動物實驗中我們發現 TB 可以明顯的抑制裸鼠的 A431 腫瘤生長，在組織切片中 A431 腫瘤以 TB 治療之後並略為增加了細胞凋亡的現象，而其角質層明顯的增加了。而 p21Cip1 和 p27Kip1 在腫瘤上的表現的區域也有明顯的不同， p21Cip1 主要表現在分化較差的區域，而 p27Kip1 則在分化較好的區域表現較多。當以不同濃度的 TB 處理 A431 細胞時，隨著 TB 濃度的增加， p21 Cip1 、 p27Kip1 和 Procaspase-3 的表現也隨著濃度而增加了，抗細胞凋亡的 Bcl-2 的表現則是減少了。 p21Cip1 在附著和自然漂浮的細胞的表現則是和動物實驗中有非常類似的結果，其表現以在附著的細胞有隨 TB 劑量而增加表現的現象，而在自然漂浮的細胞則是幾乎沒有表現的。不過 p27Kip1 的表現量在附著和自然漂浮的細胞沒有明顯的差異

，但在自然漂浮的細胞有 degradation 的現象。 Bcl-2 的表現以在附著的細胞表現較自然漂浮的細胞為多，但在以 100 uM TB 處理時則恰好相反。 Involucrin 在自然漂浮的細胞雖然在總表現量上沒有明顯差異，不過其 degrade form 的表現卻是減少了。在懸浮式培養時 p27Kip1 的表現同樣也隨著 TB 的劑量而增加， Bcl-2 的表現則幾乎看不到。在以不同劑量的 TB 處理細胞後，角質細胞分化的 Loricrin 和 Transglutaminase-1 (TGase-1) 的基因轉錄都增加了，在 TB 處理後自然漂浮的 A431 細胞，同樣有增加的趨勢。在此我們發現， TB 可能經由增加 p21Cip1 和 p27Kip1 及抑制 Bcl-2 表現的機制，以增加 A4 31 細胞分化和細胞凋亡的現象，而抑制了其增生的機制。

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Studies on the Mechanism of Terbinafine-induced Anti-Proliferation Eff ects in Human Epidermal Carcinoma (A431) Cells.

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In this study, we demonstrated Terbinafine (TB), the widely used oral- antifungal a

gents, induces differentiation in human epidermal cancer (A431) cells. TB inhibited

the growth of A431 tumor significantly. In TB treated A431 tumor, more p21Cip1

expressed in the less differentiated A431 tumor region, however p27Kip1 was detec

Terbinafine 抑制人類上皮癌細胞﹙ A431﹚ 生長機制之研究

Terbinafine

In this study, we demonstrated Terbinafine (TB), the widely used oral- antifungal a

gents, induces differentiation in human epidermal cancer (A431) cells. TB inhibited

the growth of A431 tumor significantly. In TB treated A431 tumor, more p21Cip1

expressed in the less differentiated A431 tumor region, however p27Kip1 was detec

ted more in the well differentiated region. TB increased the expression of p21Cip1

and p27Kip1 expression but decreased the expression of Bcl-2 in A431 cells. TB in

duced the expression of p21Cip1 in attached A431 cells but not in detached ones. T

he expression of p27Kip1 was also elevated after the treatment of TB. TB decrease

d the expression of Bcl-2 which most expressed in the attached A431 cells. In contr

ast, procaspase-3 expression in attached A431 cells was rised after the TB treatmen

t (25 uM), and the activation of caspase-3 occurred in 100 uM TB treated detached

A431 cells. TB also upregulates both mRNA of loricrin and tranglutaminase-1 (TG

ase-1) which belong to late-stage keratinocyte differentiation markers. After the tre

atment of TB, the transcription of loricrin and TGase-1 in detached A431 cells wer

e increased, but decreased in attached ones. Our results indicates that TB plays anot

her role in promoting tumor cell differentiation as a potential cancer chemotherape

utic agents.