Kearsley Jh scite author profile

We have previously described the establishment of a number of cell lines from Merkel cell carcinoma (MCC), also known as small cell cancer of the skin or neuroendocrine carcinoma of the skin. These cells, all of which grew as suspension cultures, were found to resemble small cell lung cancer (SCLC) lines types 1, 2 and 3 by their morphology and growth characteristics. We now report 4 more MCC cell lines which resemble the SCLC type 4 cell lines in that they grow as adherent monolayers. These MCC lines would belong to the variant subgroup as they no longer express most neuroendocrine markers, grow at low cell density and have population doubling times of 1-5 days in contrast to the MCC suspension lines which have doubling times of 6-12 days. MCC14/1 and MCC14/2 were established from the same metastatic node and would appear to represent 2 clones of the tumour which differ in morphology, histochemical markers and DNA content. We present details of the morphology, DNA content and immunohistochemistry of these 4 lines and compare their growth patterns with those of SCLC and MCC lines which grow in suspension.

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An immunohistochemical assessment of cellular proliferation markers in head and neck squamous cell cancers

Furlong²,

Cooke³

et al. 1990

Br J Cancer

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Analysis of gene amplification in head‐and‐neck squamous‐cell carcinomas

Chenevix-Trench

et al. 1991

Intl Journal of Cancer

111

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The presence of gene amplification was determined in 66 fresh head-and-neck SCC specimens using a battery of 9 different probes. Amplification of at least one gene was found in 12 samples (18%), of which 7 were amplified at multiple loci (58%). We observed amplifications for EGFR (10% of samples) and c-myc (9%), as well as co-amplification of bcl-1/int-2 (7%). No amplifications were demonstrated for c-Ha-ras-1, TGF alpha, c-mos, c-erbB-2, or c-erbA-2. The incidence of proto-oncogene amplification in head-and-neck SCC patients is comparable to that reported for other solid tumours. There was no statistically significant difference in survival between patients with or without gene amplification. However, the presence of multiple amplifications in several patients with advanced primary tumours suggests that the accumulation of genetic changes may correlate more closely with tumour size than with inherent biologic aggression.

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Malignant phyllodes tumours of the breast display increased stromal p53 protein expression

Millar

Beretov²,

Marr³

et al. 1999

Histopathology

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Chromosomes 1, 11, and 13 are frequently involved in karyotypic abnormalities in metastatic Merkel cell carcinoma

Leonard

1993

Cancer Genetics and Cytogenetics

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Kearsley Jh

Characterisation of four merkel cell carcinoma adherent cell lines

An immunohistochemical assessment of cellular proliferation markers in head and neck squamous cell cancers

Analysis of gene amplification in head‐and‐neck squamous‐cell carcinomas

Malignant phyllodes tumours of the breast display increased stromal p53 protein expression

Chromosomes 1, 11, and 13 are frequently involved in karyotypic abnormalities in metastatic Merkel cell carcinoma

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