Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma

BACKGROUND: The ability of recombinant antibodies to adequately penetrate into tumours is a key factor in achieving therapeutic effect; however, the behaviour of antibodies at a cellular level in tumours is poorly understood. The purpose of this study was to investigate those factors that influence...

Descripción completa

Detalles Bibliográficos
Autores principales: Ciprotti, Marika, Chong, Geoffrey, Gan, Hui K, Chan, Anthony, Murone, Carmel, MacGregor, Duncan, Lee, Fook-Thean, Johns, Terrance G, Heath, Joan K, Ernst, Matthias, Burgess, Antony W, Scott, Andrew M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer 2014
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4070025/
https://www.ncbi.nlm.nih.gov/pubmed/24995151
http://dx.doi.org/10.1186/s13550-014-0022-x
_version_ 1782322628485185536
author Ciprotti, Marika
Chong, Geoffrey
Gan, Hui K
Chan, Anthony
Murone, Carmel
MacGregor, Duncan
Lee, Fook-Thean
Johns, Terrance G
Heath, Joan K
Ernst, Matthias
Burgess, Antony W
Scott, Andrew M
author_facet Ciprotti, Marika
Chong, Geoffrey
Gan, Hui K
Chan, Anthony
Murone, Carmel
MacGregor, Duncan
Lee, Fook-Thean
Johns, Terrance G
Heath, Joan K
Ernst, Matthias
Burgess, Antony W
Scott, Andrew M
author_sort Ciprotti, Marika
collection PubMed
description BACKGROUND: The ability of recombinant antibodies to adequately penetrate into tumours is a key factor in achieving therapeutic effect; however, the behaviour of antibodies at a cellular level in tumours is poorly understood. The purpose of this study was to investigate those factors that influence the macroscopic and microscopic intratumoural distribution of an IgG1-humanized antibody, huA33, in colorectal tumours. METHODS: Twelve patients were infused with radiolabelled huA33 at 7 days prior to elective surgery for colorectal carcinoma. Macroscopic huA33 uptake was determined by both gamma well counter and autoradiography measurements of the resected tumour specimens. Microscopic uptake was then quantitated at a cellular level and compared to vascular penetrance. The impact of variation in tumour antigen (GPA33) expression, tumour size, specimen type (primary vs metastatic), presence of macroscopic necrosis, and tumour vasculature on huA33 uptake were examined. RESULTS: The I-huA33 uptake in whole tumour sections was (mean ± SD) 5.13 ± 2.71 × 10(−3)% injected dose per gram (ID/g). GPA33 was expressed in all viable tumour cells, and huA33 uptake was excellent regardless of tumour size and specimen type. In tumours with macroscopically evident central necrosis (n = 5), huA33 uptake in tumour necrotic centres was lower than in viable peripheries (0.606 ± 0.493 vs 2.98 ± 2.17 × 10(−3)%ID, p = 0.06). However, when corrected for low cell viability in necrotic centres, uptake of huA33 at the cellular level was highly comparable to that in the more viable tumour periphery (7.10 ± 5.10 × 10(−9) vs 3.82 ± 3.67 × 10(−9)%ID/cell, p = 0.4). In the five patients who exhibited macroscopic necrosis in their tumours, huA33 showed excellent tissue penetration, with a maximum penetration distance of 26 μm in peripheral tumour regions and 118 μm in central regions. No correlation was observed between (131)I-huA33 uptake in tumour on a cellular basis and tumour vascularity. CONCLUSIONS: In patients with colorectal carcinoma, monoclonal antibody huA33 effectively targets viable tumour cells in all cellular milieus examined, including effective penetration into necrotic tumour centres, a novel and therapeutically important finding.
format Online
Article
Text
id pubmed-4070025
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Springer
record_format MEDLINE/PubMed
spelling pubmed-40700252014-07-03 Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma Ciprotti, Marika Chong, Geoffrey Gan, Hui K Chan, Anthony Murone, Carmel MacGregor, Duncan Lee, Fook-Thean Johns, Terrance G Heath, Joan K Ernst, Matthias Burgess, Antony W Scott, Andrew M EJNMMI Res Original Research BACKGROUND: The ability of recombinant antibodies to adequately penetrate into tumours is a key factor in achieving therapeutic effect; however, the behaviour of antibodies at a cellular level in tumours is poorly understood. The purpose of this study was to investigate those factors that influence the macroscopic and microscopic intratumoural distribution of an IgG1-humanized antibody, huA33, in colorectal tumours. METHODS: Twelve patients were infused with radiolabelled huA33 at 7 days prior to elective surgery for colorectal carcinoma. Macroscopic huA33 uptake was determined by both gamma well counter and autoradiography measurements of the resected tumour specimens. Microscopic uptake was then quantitated at a cellular level and compared to vascular penetrance. The impact of variation in tumour antigen (GPA33) expression, tumour size, specimen type (primary vs metastatic), presence of macroscopic necrosis, and tumour vasculature on huA33 uptake were examined. RESULTS: The I-huA33 uptake in whole tumour sections was (mean ± SD) 5.13 ± 2.71 × 10(−3)% injected dose per gram (ID/g). GPA33 was expressed in all viable tumour cells, and huA33 uptake was excellent regardless of tumour size and specimen type. In tumours with macroscopically evident central necrosis (n = 5), huA33 uptake in tumour necrotic centres was lower than in viable peripheries (0.606 ± 0.493 vs 2.98 ± 2.17 × 10(−3)%ID, p = 0.06). However, when corrected for low cell viability in necrotic centres, uptake of huA33 at the cellular level was highly comparable to that in the more viable tumour periphery (7.10 ± 5.10 × 10(−9) vs 3.82 ± 3.67 × 10(−9)%ID/cell, p = 0.4). In the five patients who exhibited macroscopic necrosis in their tumours, huA33 showed excellent tissue penetration, with a maximum penetration distance of 26 μm in peripheral tumour regions and 118 μm in central regions. No correlation was observed between (131)I-huA33 uptake in tumour on a cellular basis and tumour vascularity. CONCLUSIONS: In patients with colorectal carcinoma, monoclonal antibody huA33 effectively targets viable tumour cells in all cellular milieus examined, including effective penetration into necrotic tumour centres, a novel and therapeutically important finding. Springer 2014-05-30 /pmc/articles/PMC4070025/ /pubmed/24995151 http://dx.doi.org/10.1186/s13550-014-0022-x Text en Copyright © 2014 Ciprotti et al.; licensee Springer http://creativecommons.org/licenses/by/4.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research
Ciprotti, Marika
Chong, Geoffrey
Gan, Hui K
Chan, Anthony
Murone, Carmel
MacGregor, Duncan
Lee, Fook-Thean
Johns, Terrance G
Heath, Joan K
Ernst, Matthias
Burgess, Antony W
Scott, Andrew M
Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title_full Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title_fullStr Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title_full_unstemmed Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title_short Quantitative intratumoural microdistribution and kinetics of (131)I-huA33 antibody in patients with colorectal carcinoma
title_sort quantitative intratumoural microdistribution and kinetics of (131)i-hua33 antibody in patients with colorectal carcinoma
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4070025/
https://www.ncbi.nlm.nih.gov/pubmed/24995151
http://dx.doi.org/10.1186/s13550-014-0022-x
work_keys_str_mv AT ciprottimarika quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT chonggeoffrey quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT ganhuik quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT chananthony quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT muronecarmel quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT macgregorduncan quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT leefookthean quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT johnsterranceg quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT heathjoank quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT ernstmatthias quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT burgessantonyw quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma
AT scottandrewm quantitativeintratumouralmicrodistributionandkineticsof131ihua33antibodyinpatientswithcolorectalcarcinoma

Ejemplares similares