Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema

SIMPLE SUMMARY: Lymphedema is a common complication of cancer, and patients with lymphedema have substantially decreased quality of life and suffer from lifelong symptoms. This study aimed to examine the effect of inhibition of Th2 inflammation in lymphedema by using QBX258, a combination of IL4/13...

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Autores principales: Mehrara, Babak J., Park, Hyeung Ju, Kataru, Raghu P., Bromberg, Jacqueline, Coriddi, Michelle, Baik, Jung Eun, Shin, Jinyeon, Li, Claire, Cavalli, Michele R., Encarnacion, Elizabeth M., Lee, Meghan, Van Zee, Kimberly J., Riedel, Elyn, Dayan, Joseph H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8466465/
https://www.ncbi.nlm.nih.gov/pubmed/34571811
http://dx.doi.org/10.3390/biology10090934
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author Mehrara, Babak J.
Park, Hyeung Ju
Kataru, Raghu P.
Bromberg, Jacqueline
Coriddi, Michelle
Baik, Jung Eun
Shin, Jinyeon
Li, Claire
Cavalli, Michele R.
Encarnacion, Elizabeth M.
Lee, Meghan
Van Zee, Kimberly J.
Riedel, Elyn
Dayan, Joseph H.
author_facet Mehrara, Babak J.
Park, Hyeung Ju
Kataru, Raghu P.
Bromberg, Jacqueline
Coriddi, Michelle
Baik, Jung Eun
Shin, Jinyeon
Li, Claire
Cavalli, Michele R.
Encarnacion, Elizabeth M.
Lee, Meghan
Van Zee, Kimberly J.
Riedel, Elyn
Dayan, Joseph H.
author_sort Mehrara, Babak J.
collection PubMed
description SIMPLE SUMMARY: Lymphedema is a common complication of cancer, and patients with lymphedema have substantially decreased quality of life and suffer from lifelong symptoms. This study aimed to examine the effect of inhibition of Th2 inflammation in lymphedema by using QBX258, a combination of IL4/13 neutralizing antibodies. QBX258 treatment increased quality of life and reduced pathologic changes in skin including hyperkeratosis, cytokine production, fibrosis and immune cell recruitment. In conclusion, this study suggested that immunotherapy against IL4/13 improved patients’ daily life which might be related with reduced pathological skin changes. ABSTRACT: Recent studies suggest that Th2 cells play a key role in the pathology of secondary lymphedema by elaborating cytokines such as IL4 and IL13. The aim of this study was to test the efficacy of QBX258, a monoclonal IL4/IL13 neutralizing antibody, in women with breast cancer–related lymphedema (BCRL). We enrolled nine women with unilateral stage I/II BCRL and treated them once monthly with intravenous infusions of QBX258 for 4 months. We measured limb volumes, bioimpedance, and skin tonometry, and analyzed the quality of life (QOL) using a validated lymphedema questionnaire (Upper Limb Lymphedema 27, ULL-27) before treatment, immediately after treatment, and 4 months following treatment withdrawal. We also obtained 5 mm skin biopsies from the normal and lymphedematous limbs before and after treatment. Treatment was well-tolerated; however, one patient with a history of cellulitis developed cellulitis during the trial and was excluded from further analysis. We found no differences in limb volumes or bioimpedance measurements after drug treatment. However, QBX258 treatment improved skin stiffness (p < 0.001) and improved QOL measurements (Physical p < 0.05, Social p = 0.01). These improvements returned to baseline after treatment withdrawal. Histologically, treatment decreased epidermal thickness, the number of proliferating keratinocytes, type III collagen deposition, infiltration of mast cells, and the expression of Th2-inducing cytokines in the lymphedematous skin. Our limited study suggests that immunotherapy against Th2 cytokines may improve skin changes and QOL of women with BCRL. This treatment appears to be less effective for decreasing limb volumes; however, additional studies are needed.
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spelling pubmed-84664652021-09-27 Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema Mehrara, Babak J. Park, Hyeung Ju Kataru, Raghu P. Bromberg, Jacqueline Coriddi, Michelle Baik, Jung Eun Shin, Jinyeon Li, Claire Cavalli, Michele R. Encarnacion, Elizabeth M. Lee, Meghan Van Zee, Kimberly J. Riedel, Elyn Dayan, Joseph H. Biology (Basel) Article SIMPLE SUMMARY: Lymphedema is a common complication of cancer, and patients with lymphedema have substantially decreased quality of life and suffer from lifelong symptoms. This study aimed to examine the effect of inhibition of Th2 inflammation in lymphedema by using QBX258, a combination of IL4/13 neutralizing antibodies. QBX258 treatment increased quality of life and reduced pathologic changes in skin including hyperkeratosis, cytokine production, fibrosis and immune cell recruitment. In conclusion, this study suggested that immunotherapy against IL4/13 improved patients’ daily life which might be related with reduced pathological skin changes. ABSTRACT: Recent studies suggest that Th2 cells play a key role in the pathology of secondary lymphedema by elaborating cytokines such as IL4 and IL13. The aim of this study was to test the efficacy of QBX258, a monoclonal IL4/IL13 neutralizing antibody, in women with breast cancer–related lymphedema (BCRL). We enrolled nine women with unilateral stage I/II BCRL and treated them once monthly with intravenous infusions of QBX258 for 4 months. We measured limb volumes, bioimpedance, and skin tonometry, and analyzed the quality of life (QOL) using a validated lymphedema questionnaire (Upper Limb Lymphedema 27, ULL-27) before treatment, immediately after treatment, and 4 months following treatment withdrawal. We also obtained 5 mm skin biopsies from the normal and lymphedematous limbs before and after treatment. Treatment was well-tolerated; however, one patient with a history of cellulitis developed cellulitis during the trial and was excluded from further analysis. We found no differences in limb volumes or bioimpedance measurements after drug treatment. However, QBX258 treatment improved skin stiffness (p < 0.001) and improved QOL measurements (Physical p < 0.05, Social p = 0.01). These improvements returned to baseline after treatment withdrawal. Histologically, treatment decreased epidermal thickness, the number of proliferating keratinocytes, type III collagen deposition, infiltration of mast cells, and the expression of Th2-inducing cytokines in the lymphedematous skin. Our limited study suggests that immunotherapy against Th2 cytokines may improve skin changes and QOL of women with BCRL. This treatment appears to be less effective for decreasing limb volumes; however, additional studies are needed. MDPI 2021-09-18 /pmc/articles/PMC8466465/ /pubmed/34571811 http://dx.doi.org/10.3390/biology10090934 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Mehrara, Babak J.
Park, Hyeung Ju
Kataru, Raghu P.
Bromberg, Jacqueline
Coriddi, Michelle
Baik, Jung Eun
Shin, Jinyeon
Li, Claire
Cavalli, Michele R.
Encarnacion, Elizabeth M.
Lee, Meghan
Van Zee, Kimberly J.
Riedel, Elyn
Dayan, Joseph H.
Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title_full Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title_fullStr Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title_full_unstemmed Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title_short Pilot Study of Anti-Th2 Immunotherapy for the Treatment of Breast Cancer-Related Upper Extremity Lymphedema
title_sort pilot study of anti-th2 immunotherapy for the treatment of breast cancer-related upper extremity lymphedema
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8466465/
https://www.ncbi.nlm.nih.gov/pubmed/34571811
http://dx.doi.org/10.3390/biology10090934
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