Department of Laboratory Medicine, University of Padova, Padova, Italy.
Pancreas. 2010 Jul;39(5):662-8. doi: 10.1097/MPA.0b013e3181c8b48c.
alpha-Tocopheryl succinate (alpha-TOS) is thought to be toxic only for cancer cells. We ascertained in vitro alpha-TOS effects on pancreatic cancer (PC) and normal cell growth and verified whether the combination of nontoxic alpha-TOS and 5-fluorouracil (5-FU) doses causes cancer cell death and whether alpha-TOS effects are mediated by the proapoptotic proteins Bax/Bak and/or SMAD4/DPC4 status.
Five PC cell lines, myoblasts, normal monocytes, wild-type (WT) and Bax/Bak double knockout mouse embryonic fibroblast (MEF) cells, and permanently SMAD4/DPC4-transfected PSN1 cells were cultured in 1% and 10% fetal calf serums (FCSs), without or with alpha-TOS (5-500 micromol/L). Nontoxic 5-FU (0.0001 mmol/L) and alpha-TOS alone or in combination were also evaluated.
Only PSN1 PC cell line, which had SMAD4/DPC4 homozygous deletion, was sensitive to nontoxic alpha-TOS doses (5 micromol/L in 1% FCS and 50 micromol/L in 10% FCS). A 20-micromol/L alpha-TOS inhibited MEF-WT, not MEF-double knockout growth. Only PSN1 cells were sensitive to nontoxic 5-FU and alpha-TOS combination. SMAD4/DPC4 transfection restored PSN1 resistance to the effects of combined 5-FU and alpha-TOS effects.
Only a minority of PC cells are sensitive to the antiproliferative effects of alpha-TOS, any sensitivity appearing to be correlated with SMAD4/DPC4 homozygous deletion and Bax/Bak expression.
α-生育酚琥珀酸酯(α-TOS)被认为仅对癌细胞有毒。我们在体外确定了 α-TOS 对胰腺癌(PC)和正常细胞生长的影响,并验证了无毒的 α-TOS 与 5-氟尿嘧啶(5-FU)剂量的组合是否会导致癌细胞死亡,以及 α-TOS 的作用是否通过促凋亡蛋白 Bax/Bak 和/或 SMAD4/DPC4 状态介导。
培养了 5 种 PC 细胞系、成肌细胞、正常单核细胞、野生型(WT)和 Bax/Bak 双敲除小鼠胚胎成纤维细胞(MEF)以及永久性 SMAD4/DPC4 转染的 PSN1 细胞,在 1%和 10%胎牛血清(FCS)中,有无 α-TOS(5-500 μmol/L)。还评估了无毒的 5-FU(0.0001 mmol/L)和单独的 α-TOS 或联合应用。
只有具有 SMAD4/DPC4 纯合缺失的 PSN1 PC 细胞系对无毒的 α-TOS 剂量(1% FCS 中的 5 μmol/L 和 10% FCS 中的 50 μmol/L)敏感。20 μmol/L 的 α-TOS 抑制 MEF-WT,但不抑制 MEF 双敲除细胞的生长。只有 PSN1 细胞对无毒的 5-FU 和 α-TOS 联合敏感。SMAD4/DPC4 转染恢复了 PSN1 对联合 5-FU 和 α-TOS 作用的耐药性。
只有少数 PC 细胞对 α-TOS 的增殖抑制作用敏感,任何敏感性似乎都与 SMAD4/DPC4 纯合缺失和 Bax/Bak 表达相关。