Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy

Intraperitoneal (211)At-based targeted α-therapy (TAT) may hold great promise as an adjuvant therapy after surgery and chemotherapy in epithelial ovarian cancer to eradicate any remaining undetectable disease. This implies that it will also be delivered to patients possibly already cured by the prim...

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Autores principales: Leidermark, Erik, Hallqvist, Andreas, Jacobsson, Lars, Karlsson, Per, Holmberg, Erik, Bäck, Tom, Johansson, Mia, Lindegren, Sture, Palm, Stig, Albertsson, Per
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society of Nuclear Medicine 2023
Materias:
Clinical Investigation
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9841246/
https://www.ncbi.nlm.nih.gov/pubmed/35798559
http://dx.doi.org/10.2967/jnumed.121.263349
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author Leidermark, Erik
Hallqvist, Andreas
Jacobsson, Lars
Karlsson, Per
Holmberg, Erik
Bäck, Tom
Johansson, Mia
Lindegren, Sture
Palm, Stig
Albertsson, Per
author_facet Leidermark, Erik
Hallqvist, Andreas
Jacobsson, Lars
Karlsson, Per
Holmberg, Erik
Bäck, Tom
Johansson, Mia
Lindegren, Sture
Palm, Stig
Albertsson, Per
author_sort Leidermark, Erik
collection PubMed
description Intraperitoneal (211)At-based targeted α-therapy (TAT) may hold great promise as an adjuvant therapy after surgery and chemotherapy in epithelial ovarian cancer to eradicate any remaining undetectable disease. This implies that it will also be delivered to patients possibly already cured by the primary treatment. An estimate of long-term risks is therefore sought to determine whether the treatment is justified. Methods: Baseline data for risk estimates of α-particle irradiation were collected from published studies on excess cancer induction and mortality for subjects exposed to either (224)Ra treatments or Thorotrast contrast agent (25% ThO(2) colloid, containing (232)Th). Organ dosimetry for (224)Ra and Thorotrast irradiation were taken from the literature. These organ-specific risks were then applied to our previously reported dosimetry for intraperitoneal (211)At-TAT patients. Results: Risk could be estimated for 10 different organ or organ groups. The calculated excess relative risk per gray (ERR/Gy) could be sorted into 2 groups. The lower-ERR/Gy group, ranging up to a value of approximately 5, included trachea, bronchus, and lung, at 0.52 (95% CI, 0.21–0.82); stomach, at 1.4 (95% CI, −5.0–7.9); lymphoid and hematopoietic system, at 2.17 (95% CI, 1.7–2.7); bone and articular cartilage, at 2.6 (95% CI, 2.0–3.3); breast, at 3.45 (95% CI, −10–17); and colon, at 4.5 (95% CI, −3.5–13). The higher-ERR/Gy group, ranging from approximately 10 to 15, included urinary bladder, at 10.1 (95% CI, 1.4–23); liver, at 14.2 (95% CI, 13–16); kidney, at 14.9 (95% CI, 3.9–26); and lip, oral cavity, and pharynx, at 15.20 (95% CI, 2.73–27.63). Applying a typical candidate patient (female, age 65 y) and correcting for the reference population mortality rate, the total estimated excess mortality for an intraperitoneal (211)At-monoclonal antibody treatment amounted to 1.13 per 100 treated. More than half this excess originated from urinary bladder and kidney, 0.29 and 0.34, respectively. Depending on various adjustments in calculation and assumptions on competing risks, excess mortality could range from 0.11 to 1.84 per 100 treated. Conclusion: Published epidemiologic data on lifelong detriment after α-particle irradiation and its dosimetry allowed calculations to estimate the risk for secondary cancer after (211)At-based intraperitoneal TAT. Measures to reduce dose to the urinary organs may further decrease the estimated relative low risk for secondary cancer from (211)At-monoclonal antibody–based intraperitoneal TAT.
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spelling pubmed-98412462023-04-19 Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy Leidermark, Erik Hallqvist, Andreas Jacobsson, Lars Karlsson, Per Holmberg, Erik Bäck, Tom Johansson, Mia Lindegren, Sture Palm, Stig Albertsson, Per J Nucl Med Clinical Investigation Intraperitoneal (211)At-based targeted α-therapy (TAT) may hold great promise as an adjuvant therapy after surgery and chemotherapy in epithelial ovarian cancer to eradicate any remaining undetectable disease. This implies that it will also be delivered to patients possibly already cured by the primary treatment. An estimate of long-term risks is therefore sought to determine whether the treatment is justified. Methods: Baseline data for risk estimates of α-particle irradiation were collected from published studies on excess cancer induction and mortality for subjects exposed to either (224)Ra treatments or Thorotrast contrast agent (25% ThO(2) colloid, containing (232)Th). Organ dosimetry for (224)Ra and Thorotrast irradiation were taken from the literature. These organ-specific risks were then applied to our previously reported dosimetry for intraperitoneal (211)At-TAT patients. Results: Risk could be estimated for 10 different organ or organ groups. The calculated excess relative risk per gray (ERR/Gy) could be sorted into 2 groups. The lower-ERR/Gy group, ranging up to a value of approximately 5, included trachea, bronchus, and lung, at 0.52 (95% CI, 0.21–0.82); stomach, at 1.4 (95% CI, −5.0–7.9); lymphoid and hematopoietic system, at 2.17 (95% CI, 1.7–2.7); bone and articular cartilage, at 2.6 (95% CI, 2.0–3.3); breast, at 3.45 (95% CI, −10–17); and colon, at 4.5 (95% CI, −3.5–13). The higher-ERR/Gy group, ranging from approximately 10 to 15, included urinary bladder, at 10.1 (95% CI, 1.4–23); liver, at 14.2 (95% CI, 13–16); kidney, at 14.9 (95% CI, 3.9–26); and lip, oral cavity, and pharynx, at 15.20 (95% CI, 2.73–27.63). Applying a typical candidate patient (female, age 65 y) and correcting for the reference population mortality rate, the total estimated excess mortality for an intraperitoneal (211)At-monoclonal antibody treatment amounted to 1.13 per 100 treated. More than half this excess originated from urinary bladder and kidney, 0.29 and 0.34, respectively. Depending on various adjustments in calculation and assumptions on competing risks, excess mortality could range from 0.11 to 1.84 per 100 treated. Conclusion: Published epidemiologic data on lifelong detriment after α-particle irradiation and its dosimetry allowed calculations to estimate the risk for secondary cancer after (211)At-based intraperitoneal TAT. Measures to reduce dose to the urinary organs may further decrease the estimated relative low risk for secondary cancer from (211)At-monoclonal antibody–based intraperitoneal TAT. Society of Nuclear Medicine 2023-01 /pmc/articles/PMC9841246/ /pubmed/35798559 http://dx.doi.org/10.2967/jnumed.121.263349 Text en © 2023 by the Society of Nuclear Medicine and Molecular Imaging. https://creativecommons.org/licenses/by/4.0/Immediate Open Access: Creative Commons Attribution 4.0 International License (CC BY) allows users to share and adapt with attribution, excluding materials credited to previous publications. License: https://creativecommons.org/licenses/by/4.0/. Details: http://jnm.snmjournals.org/site/misc/permission.xhtml.
spellingShingle Clinical Investigation
Leidermark, Erik
Hallqvist, Andreas
Jacobsson, Lars
Karlsson, Per
Holmberg, Erik
Bäck, Tom
Johansson, Mia
Lindegren, Sture
Palm, Stig
Albertsson, Per
Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title_full Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title_fullStr Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title_full_unstemmed Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title_short Estimating the Risk for Secondary Cancer After Targeted α-Therapy with (211)At Intraperitoneal Radioimmunotherapy
title_sort estimating the risk for secondary cancer after targeted α-therapy with (211)at intraperitoneal radioimmunotherapy
topic Clinical Investigation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9841246/
https://www.ncbi.nlm.nih.gov/pubmed/35798559
http://dx.doi.org/10.2967/jnumed.121.263349
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