Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma
<p>Abstract</p> <p>Purpose</p> <p>To investigate the correlation between the expression of Epidermal Growth Factor receptor (EGFr) and the reduction of the effective doubling time (<it>T</it><sub><it>D</it></sub>) during radiotherapy...
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doaj-0dfe681c5be6451d94aa5f55fbf218fe2020-11-25T01:29:38ZengBMCRadiation Oncology1748-717X2012-08-017114310.1186/1748-717X-7-143Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinomaPedicini PiernicolaNappi AntonioStrigari LidiaAlicia Jereczek-Fossa BarbaraAlterio DanielaCremonesi MartaBotta FrancescaVischioni BarbaraCaivano RocchinaFiorentino AlbaImprota GiuseppinaStorto GiovanniBenassi MarcelloOrecchia RobertoSalvatore Marco<p>Abstract</p> <p>Purpose</p> <p>To investigate the correlation between the expression of Epidermal Growth Factor receptor (EGFr) and the reduction of the effective doubling time (<it>T</it><sub><it>D</it></sub>) during radiotherapy treatment and also to determine the dose per fraction to be taken into account when the overall treatment time (OTT) is reduced in accelerated radiotherapy of head and neck squamous cell carcinoma (HNSCC).</p> <p>Methods</p> <p>A survey of the published papers comparing 3-years of local regional control rate (LCR) for a total of 2162 patients treated with conventional and accelerated radiotherapy and with a pretreatment assessment of EGFr expression, was made. Different values of <it>T</it><sub><it>D</it></sub> were obtained by a model incorporating the overall time corrected biologically effective dose (<it>BED</it>) and a 3-year clinical LCR for high and low EGFr groups of patients (H<sub>EGFr</sub> and L<sub>EGFr</sub>), respectively. By obtaining the <it>T</it><sub><it>D</it></sub> from the above analysis and the sub-sites’ potential doubling time (<it>T</it><sub><it>pot</it></sub>) from flow cytometry and immunohistochemical methods, we were able to estimate the average <it>T</it><sub><it>D</it></sub> for each sub-site included in the analysis. Moreover, the dose that would be required to offset the modified proliferation occurring in one day (<it>D</it><sub><it>prolif</it></sub>), was estimated.</p> <p>Results</p> <p>The averages of <it>T</it><sub><it>D</it></sub> were 77 (27-90)<sub>95%</sub> days in L<sub>EGFr</sub> and 8.8 (7.3-11.0)<sub>95%</sub> days in H<sub>EGFr</sub>, if an onset of accelerated proliferation <it>T</it><sub><it>K</it></sub> at day 21 was assumed. The correspondent H<sub>EGFr</sub> sub-sites’ <it>T</it><sub><it>D</it></sub> were 5.9 (6.6), 5.9 (6.6), 4.6 (6.1), 14.3 (12.9) days, with respect to literature immunohistochemical (flow cytometry) data of <it>T</it><sub><it>pot</it></sub> for Oral-Cavity, Oro-pharynx, Hypo-pharynx, and Larynx respectively. The <it>D</it><sub><it>prolif</it></sub> for the H<sub>EGFr</sub> groups were 0.33 (0.29), 0.33 (0.29), 0.42 (0.31), 0.14 (0.15) Gy/day if <it>α</it> = 0.3 Gy<sup>-1</sup> and <it>α/β</it> = 10 Gy were assumed.</p> <p>Conclusions</p> <p>A higher expression of the EGFr leads to enhanced proliferation. This study allowed to quantify the extent of the effect which EGFr expression has in terms of reduced <it>T</it><sub><it>D</it></sub> and <it>D</it><sub><it>prolif</it></sub> for each head and neck sub-site.</p> http://www.ro-journal.com/content/7/1/143EGFrDoubling timePotential doubling timeCell loss factor |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Pedicini Piernicola Nappi Antonio Strigari Lidia Alicia Jereczek-Fossa Barbara Alterio Daniela Cremonesi Marta Botta Francesca Vischioni Barbara Caivano Rocchina Fiorentino Alba Improta Giuseppina Storto Giovanni Benassi Marcello Orecchia Roberto Salvatore Marco |
spellingShingle |
Pedicini Piernicola Nappi Antonio Strigari Lidia Alicia Jereczek-Fossa Barbara Alterio Daniela Cremonesi Marta Botta Francesca Vischioni Barbara Caivano Rocchina Fiorentino Alba Improta Giuseppina Storto Giovanni Benassi Marcello Orecchia Roberto Salvatore Marco Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma Radiation Oncology EGFr Doubling time Potential doubling time Cell loss factor |
author_facet |
Pedicini Piernicola Nappi Antonio Strigari Lidia Alicia Jereczek-Fossa Barbara Alterio Daniela Cremonesi Marta Botta Francesca Vischioni Barbara Caivano Rocchina Fiorentino Alba Improta Giuseppina Storto Giovanni Benassi Marcello Orecchia Roberto Salvatore Marco |
author_sort |
Pedicini Piernicola |
title |
Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
title_short |
Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
title_full |
Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
title_fullStr |
Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
title_full_unstemmed |
Correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
title_sort |
correlation between egfr expression and accelerated proliferation during radiotherapy of head and neck squamous cell carcinoma |
publisher |
BMC |
series |
Radiation Oncology |
issn |
1748-717X |
publishDate |
2012-08-01 |
description |
<p>Abstract</p> <p>Purpose</p> <p>To investigate the correlation between the expression of Epidermal Growth Factor receptor (EGFr) and the reduction of the effective doubling time (<it>T</it><sub><it>D</it></sub>) during radiotherapy treatment and also to determine the dose per fraction to be taken into account when the overall treatment time (OTT) is reduced in accelerated radiotherapy of head and neck squamous cell carcinoma (HNSCC).</p> <p>Methods</p> <p>A survey of the published papers comparing 3-years of local regional control rate (LCR) for a total of 2162 patients treated with conventional and accelerated radiotherapy and with a pretreatment assessment of EGFr expression, was made. Different values of <it>T</it><sub><it>D</it></sub> were obtained by a model incorporating the overall time corrected biologically effective dose (<it>BED</it>) and a 3-year clinical LCR for high and low EGFr groups of patients (H<sub>EGFr</sub> and L<sub>EGFr</sub>), respectively. By obtaining the <it>T</it><sub><it>D</it></sub> from the above analysis and the sub-sites’ potential doubling time (<it>T</it><sub><it>pot</it></sub>) from flow cytometry and immunohistochemical methods, we were able to estimate the average <it>T</it><sub><it>D</it></sub> for each sub-site included in the analysis. Moreover, the dose that would be required to offset the modified proliferation occurring in one day (<it>D</it><sub><it>prolif</it></sub>), was estimated.</p> <p>Results</p> <p>The averages of <it>T</it><sub><it>D</it></sub> were 77 (27-90)<sub>95%</sub> days in L<sub>EGFr</sub> and 8.8 (7.3-11.0)<sub>95%</sub> days in H<sub>EGFr</sub>, if an onset of accelerated proliferation <it>T</it><sub><it>K</it></sub> at day 21 was assumed. The correspondent H<sub>EGFr</sub> sub-sites’ <it>T</it><sub><it>D</it></sub> were 5.9 (6.6), 5.9 (6.6), 4.6 (6.1), 14.3 (12.9) days, with respect to literature immunohistochemical (flow cytometry) data of <it>T</it><sub><it>pot</it></sub> for Oral-Cavity, Oro-pharynx, Hypo-pharynx, and Larynx respectively. The <it>D</it><sub><it>prolif</it></sub> for the H<sub>EGFr</sub> groups were 0.33 (0.29), 0.33 (0.29), 0.42 (0.31), 0.14 (0.15) Gy/day if <it>α</it> = 0.3 Gy<sup>-1</sup> and <it>α/β</it> = 10 Gy were assumed.</p> <p>Conclusions</p> <p>A higher expression of the EGFr leads to enhanced proliferation. This study allowed to quantify the extent of the effect which EGFr expression has in terms of reduced <it>T</it><sub><it>D</it></sub> and <it>D</it><sub><it>prolif</it></sub> for each head and neck sub-site.</p> |
topic |
EGFr Doubling time Potential doubling time Cell loss factor |
url |
http://www.ro-journal.com/content/7/1/143 |
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