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苯并(a)芘转化的3T3细胞生长的控制

Control of growth of benzo(a)pyrene-transformed 3T3 cells.

作者信息

Holley R W, Baldwin J H, Kiernan J A, Messmer T O

出版信息

Proc Natl Acad Sci U S A. 1976 Sep;73(9):3229-32. doi: 10.1073/pnas.73.9.3229.

Abstract

The growth controls observed in benzo[a]pyrene-transformed 3T3 cells (BP3T3) are compared with those of virus-transformed and normal 3T3 cells. Superficially, the chemically transformed BP3T3 cells have the same behavior as virus-transformed SV3T3 cells. Both grow to high cell density in culture medium with 10% serum, both form colonies in Methocel, and both are tumorigenic. Closer examination, however, has disclosed that BP3T3 cells exhibit "normal" growth controls at low serum concentrations. In contrast to the behavior of SV3T3 cells, the initiation of DNA synthesis in BP3T3 cells is still dependent on a serum factor. If BP3T3 cells are grown in medium with 0.2% serum, the cells become quiescent, with growth arrested in the Gu or G0 phase of the cell cycle. The addition of serum or the fibroblast growth factor (FGF) to such quiescent cells leads to the initiation of DNA synthesis and the resumption of growth. As with normal 3T3 cells, if the growth rate of BP3T3 cells is limited by a suboptimal concentration of serum, the growth rate of the cells is increased by the addition of FGF. Also, BP3T3 cells show density-dependent regulation of growth, if the medium contains a low concentration of serum. BP3T3 cells, therefore, have the behavior of "transformed" cells when cultured in medium with 10% serum, but behave as "normal" cells in medium with low serum. In comparison with normal 3T3 cells, the difference in growth behavior of BP3T3 cells appears to be due to a substantial decrease in the cells' requirement for a serum growth factor of the FGF type. Exploration of possible causes of this substantial decrease indicates that the primary cause is a lower rate of depletion of the serum growth factor from the culture medium by BP3T3 cells. The decrease in rate of depletion is sufficient to account for the uncontrolled growth of BP3T3 cells in medium with 10% serum. It is suggested that a decreased rate of depletion of a growth factor may contribute to tumorigenicity of cells in vivo.

摘要

将苯并[a]芘转化的3T3细胞(BP3T3)中观察到的生长控制与病毒转化的和正常的3T3细胞的生长控制进行比较。表面上,化学转化的BP3T3细胞与病毒转化的SV3T3细胞具有相同的行为。两者在含10%血清的培养基中都能生长到高细胞密度,两者在甲基纤维素中都能形成集落,并且两者都具有致瘤性。然而,进一步研究发现,BP3T3细胞在低血清浓度下表现出“正常”的生长控制。与SV3T3细胞的行为不同,BP3T3细胞中DNA合成的起始仍然依赖于一种血清因子。如果BP3T3细胞在含0.2%血清的培养基中生长,细胞会进入静止状态,生长停滞在细胞周期的G1或G0期。向这些静止细胞中添加血清或成纤维细胞生长因子(FGF)会导致DNA合成的起始和生长的恢复。与正常3T3细胞一样,如果BP3T3细胞的生长速率受到血清浓度不足的限制,添加FGF会提高细胞的生长速率。此外,如果培养基中含有低浓度血清,BP3T3细胞会表现出密度依赖性生长调节。因此,BP3T3细胞在含10%血清的培养基中培养时具有“转化”细胞的行为,但在低血清培养基中表现为“正常”细胞。与正常3T3细胞相比,BP3T3细胞生长行为的差异似乎是由于细胞对FGF类型血清生长因子的需求大幅降低。对这种大幅降低的可能原因的探究表明,主要原因是BP3T3细胞从培养基中消耗血清生长因子的速率较低。消耗速率的降低足以解释BP3T3细胞在含10%血清的培养基中不受控制的生长。有人提出,生长因子消耗速率的降低可能有助于体内细胞的致瘤性。

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Control of growth of benzo(a)pyrene-transformed 3T3 cells.苯并(a)芘转化的3T3细胞生长的控制
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