Richmond A, Fine R, Murray D, Lawson D H, Priest J H
J Invest Dermatol. 1986 Mar;86(3):295-302. doi: 10.1111/1523-1747.ep12285452.
It has been proposed that benign nevi that fail to differentiate normally may undergo stepwise growth and morphologic changes resulting in progression toward dysplastic nevi, which in some cases progress into malignant melanoma. In this study, we sought to determine the relationship between production of endogenous growth factors and the appearance of chromosomal abnormalities in cultured nevi and melanomas. Newly established cultures from 8 nevi with benign histology and 6 malignant melanomas, and 2 malignant melanoma cell lines were studied. Assays for mitogenic growth factors were based on stimulation of [3H]thymidine incorporation into DNA in Hs0294 malignant melanoma cells, produced by serum-free conditioned medium from nevus or melanoma cultures. Karyotypes were examined in cultures of an equivalent passage. Three of the 8 nevus cultures were mitogen-negative and displayed normal karyotypes; one nevus culture was mitogen-positive and had a normal karyotype, although the biopsied tissue demonstrated histologic evidence of benign melanocytic proliferation; one was mitogen-negative initially, but had an extra chromosome 8 in 2 of 50 cells; 3 were mitogen-positive and chromosomally abnormal. Each of the cultures in this latter group exhibited reciprocal translocation (rcpt) as the only identifiable abnormality [rcpt(6;15), rcpt(10;15), rcpt(15;20)], or a constitutional rcpt(4;5). Thus, there was direct correlation between growth factor production and chromosome abnormality in 6 of 8 benign nevus cultures. In the newly established melanoma cultures there was also concordance between growth factor and chromosomal status; conditioned media from 4 of 6 were mitogen-positive by at least one assay, and all 4 of the mitogen-positive cultures had chromosomally abnormal cell populations. Of the 2 melanoma cultures negative for growth factors, one was also negative for chromosome abnormality; the other had chromosomal change consisting of increased polyploidy. Both melanoma cell lines had abnormal karyotypes and were mitogen-positive. Though numerous chromosome changes were noted in the karyotypically abnormal melanoma cells, 6 of the 8 cultures exhibited abnormalities in chromosomes 1, 6, and/or 7. These data suggest that steps in the progression from benign nevi toward dysplastic nevi or malignant melanoma include: proliferation resulting from altered production of endogenous mitogenic growth factors; and development of specific chromosomal abnormalities.
有人提出,未能正常分化的良性痣可能会经历逐步生长和形态变化,从而发展为发育异常痣,在某些情况下,发育异常痣会进展为恶性黑色素瘤。在本研究中,我们试图确定培养的痣和黑色素瘤中内源性生长因子的产生与染色体异常出现之间的关系。我们研究了来自8例组织学良性的痣、6例恶性黑色素瘤的新建立的培养物,以及2株恶性黑色素瘤细胞系。促有丝分裂生长因子的检测基于无血清条件培养基(来自痣或黑色素瘤培养物)刺激Hs0294恶性黑色素瘤细胞将[3H]胸腺嘧啶掺入DNA。在相同传代的培养物中检查核型。8例痣培养物中有3例促有丝分裂原阴性且核型正常;1例痣培养物促有丝分裂原阳性且核型正常,但活检组织显示有良性黑素细胞增殖的组织学证据;1例最初促有丝分裂原阴性,但在50个细胞中有2个细胞有额外的8号染色体;3例促有丝分裂原阳性且染色体异常。后一组中的每个培养物都表现出相互易位(rcpt)作为唯一可识别的异常[rcpt(6;15)、rcpt(10;15)、rcpt(15;20)],或一种先天性rcpt(4;5)。因此,在8例良性痣培养物中有6例促生长因子产生与染色体异常之间存在直接相关性。在新建立的黑色素瘤培养物中,生长因子和染色体状态之间也存在一致性;6例中有4例的条件培养基通过至少一种检测促有丝分裂原呈阳性,并且所有4例促有丝分裂原阳性培养物都有染色体异常的细胞群体。在2例生长因子阴性的黑色素瘤培养物中,1例染色体异常也为阴性;另1例有包括多倍体增加的染色体变化。两株黑色素瘤细胞系核型均异常且促有丝分裂原呈阳性。虽然在核型异常的黑色素瘤细胞中发现了许多染色体变化,但8例培养物中有6例在1号、6号和/或7号染色体上出现异常。这些数据表明,从良性痣发展为发育异常痣或恶性黑色素瘤的过程包括:内源性促有丝分裂生长因子产生改变导致的增殖;以及特定染色体异常的发生。
