| Literature DB >> 21505459 |
T Bauernhofer1, M Pichler, E Wieckowski, J Stanson, A Aigelsreiter, A Griesbacher, A Groselj-Strele, A Linecker, H Samonigg, C Langner, T L Whiteside.
Abstract
BACKGROUND: The influence of human prolactin (hPRL) on the development of breast and other types of cancer is well established. Little information, however, exists on the effects of hPRL on squamous cell carcinomas of the head and neck (SCCHNs).Entities:
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Year: 2011 PMID: 21505459 PMCID: PMC3101909 DOI: 10.1038/bjc.2011.131
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Pathological characteristics of the primary and metastatic squamous cell carcinomas of the head and neck from which the respective cell lines were generated
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| PCI-4A | Larynx | Moderate |
| PCI-4B | Neck node | Moderate |
| PCI-6A | Tonsil | Well–moderate |
| PCI-6B | Neck node | Poor |
| PCI-15A | Piriform sinus | Poor |
| PCI-15B | Lymph node | Poor |
| PCI-37A | Larynx | Well–moderate |
| PCI-37B | Lymph node | Well–moderate |
Clinicopathological characteristics of the SCCHN patients included in this study
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| Male | 67 | 75% |
| Female | 22 | 25% |
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| Male | 56 (37–88) | |
| Female | 65 (40–88) | |
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| T1 | 37 | 41% |
| T2 | 21 | 24% |
| T3 | 10 | 11% |
| T4 | 21 | 24% |
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| N0 | 60 | 67% |
| N1 | 14 | 16% |
| N2 | 15 | 17% |
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| G1 | 18 | 20% |
| G2 | 46 | 52% |
| G3 | 25 | 28% |
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| I | 34 | 38% |
| II | 16 | 18% |
| III | 12 | 14% |
| IV | 27 | 30% |
Abbreviation: SCCHN=squamous cell carcinoma of the head and neck.
Surface and intracytoplasmatic expression of the PRLR on four pairs of squamous cell carcinoma lines generated from the primary tumour and autologous lymph node metastasesa
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| PCI-4A | 1 | 17 | 7 | 19 | Pos |
| PCI-4B | 6 | 38 | 16 | 21 | Pos |
| PCI-6A | 58 | 633 | 51 | 475 | Pos |
| PCI-6B | 1 | 48 | 1 | 38 | Neg |
| PCI-15A | 0 | 0 | 5 | 67 | Neg |
| PCI-15B | 0 | 0 | 2 | 80 | Neg |
| PCI-37A | 26b | 26b | 96 | 27 | Pos |
| PCI-37B | 82 | 640 | 95 | 435 | Pos |
Abbreviations: PRLR=prolactin receptor; MFI=mean fluorescence intensity; ICC=immunocytochemistry; Pos.=positive.
Data were obtained by flow cytometry of dissociated monolayers or by ICC of cytocentrifuged cells.
After trypsinization that led to considerable loss of PRLR surface expression but cells could not be detached from culture flask otherwise.
Figure 1PRLR expression in SCCHN cell lines. (A) PRLR expression measured by flow cytometry in PCI-6A, PCI-6B and T47D cell lines. The PCI-6A cell line shows a significantly higher percentage of PRLR+ cells compared with the PCI-6B cell line. (B) Immunocytochemical staining of SCCHN cell lines (magnification × 400). Positive membranous and cytoplasmic PRLR staining (red colour of Cy3) is shown for the PCI-6A cell line, whereas the PCI-6B cell line is negative. Nuclei are counterstained with Hoechst dye (blue). (C) Immunoprecipitation reveals a prominent band between 75 and 80 kD, corresponding to the PRLR protein in the lysate of PCI-6A cells, whereas only a weak band was detected in the lysate of PCI-6B cells. Immunoglobulin G (IgG) heavy chain was used as a loading control and T47D cell line served as a positive control.
Figure 2PRLR expression in SCCHN tissues. In agreement with the corresponding cell lines PCI-6A and PCI-6B, the primary tumour (A) shows PRLR positivity, whereas the metachronously developed neck lymph node metastasis (B) is PRLR negative.
Figure 3Immunohistochemistry for PRLR in SCCHN tissues. (A) Note low PRLR expression level in normal tissue and well-differentiated tumour tissue, and high PRLR expression level in poorly differentiated tumour tissue ( × 100). (B) PRLR expression on representative SCCHN spots on the TMA comprising three paired spots (columns) from four different tumours (lines). Note the variable PRLR immunoreactivity between different tumours (lines) and the high concordance between different cores from the same tumour (columns).
Figure 4Kaplan–Meier plots for overall survival (A) and disease-free survival (B) in patients with SCCHNs with low vs high PRLR expression.
Correlations between PRLR expression and clinicopathological parameters
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| T1 | 2 (25%) | 35 (43%) | 0.511 |
| T2 | 3 (37.5%) | 18 (22%) | |
| T3 | 1 (12.5%) | 9 (11) | |
| T4 | 2 (25%) | 19 (24%) | |
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| N0 | 7 (87.5%) | 53 (65%) | 0.195 |
| N1–3 | 1 (12.5%) | 28 (35%) | |
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| G1 | 3 (37.5%) | 15 (19%) | 0.404 |
| G2 | 3 (37.5%) | 43 (53%) | |
| G3 | 2 (25%) | 23 (28%) | |
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| I | 2 (37.5%) | 32 (40%) | 0.868 |
| II | 3 (37.5%) | 13 (16%) | |
| III | 1 (12%) | 11 (14%) | |
| IV | 2 (25%) | 25 (31%) | |
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| M | 5 (62%) | 62 (76%) | 0.310 |
| F | 3 (38%) | 19 (24%) | |
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| <60 | 4 (50%) | 44 (54%) | 0.551 |
| >60 | 4 (50%) | 37 (45%) | |
Abbreviation: PRLR=prolactin receptor.