Anti-oxidant vitamins reduce normal tissue toxicity induced by radio-immunotherapy

Cancer is one of the most complicated diseases in present-day medical science. Yearly, several studies suggest various strategies for preventing carcinogenesis. Furthermore, experiments for the treatment of cancer with low side effects are ongoing. Chemotherapy, targeted therapy, radiotherapy and immunotherapy are the most common non-invasive strategies for cancer treatment. One of the most challenging issues encountered with these modalities is low effectiveness, as well as normal tissue toxicity for chemo-radiation therapy. The use of some agents as adjuvants has been suggested to improve tumor responses and also alleviate normal tissue toxicity. Resveratrol, a natural flavonoid, has attracted a lot of attention for the management of both tumor and normal tissue responses to various modalities of cancer therapy. As an antioxidant and anti-inflammatory agent, in vitro and in vivo studies show that it is able to mitigate chemo-radiation toxicity in normal tissues. However, clinical studies to confirm the usage of resveratrol as a chemo-radioprotector are lacking. In addition, it can sensitize various types of cancer cells to both chemotherapy drugs and radiation. In recent years, some clinical studies suggested that resveratrol may have an effect on inducing cancer cell killing. Yet, clinical translation of resveratrol has not yielded desirable results for the combination of resveratrol with radiotherapy, targeted therapy or immunotherapy. In this paper, we review the potential role of resveratrol for preserving normal tissues and sensitization of cancer cells in combination with different cancer treatment modalities.

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Ultrasound-Mediated Gemcitabine Delivery Reduces the Normal-Tissue Toxicity of Chemoradiation Therapy in a Muscle-Invasive Bladder Cancer Model

International Journal of Radiation Oncology*Biology*Physics ◽

10.1016/j.ijrobp.2020.11.046 ◽

2021 ◽

Vol 109 (5) ◽

pp. 1472-1482 ◽

Cited By ~ 1

Author(s):

Jia-Ling Ruan ◽

Richard J. Browning ◽

Yesna O. Yildiz ◽

Michael Gray ◽

Luca Bau ◽

...

Keyword(s):

Bladder Cancer ◽

Normal Tissue ◽

Chemoradiation Therapy ◽

Invasive Bladder Cancer ◽

Cancer Model ◽

Muscle Invasive Bladder Cancer ◽

Normal Tissue Toxicity ◽

Muscle Invasive ◽

Bladder Cancer Model

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Radioimmunotherapy of PANC-1 human pancreatic cancer xenografts in NOD/SCID or NRG mice with Panitumumab labeled with Auger electron emitting, 111In or β-particle emitting, 177Lu

EJNMMI Radiopharmacy and Chemistry ◽

10.1186/s41181-020-00111-y ◽

2020 ◽

Vol 5 (1) ◽

Author(s):

Sadaf Aghevlian ◽

Zhongli Cai ◽

David Hedley ◽

Mitchell A. Winnik ◽

Raymond M. Reilly

Keyword(s):

Normal Saline ◽

Normal Tissue ◽

Auger Electron ◽

Absorbed Dose ◽

Clonogenic Survival ◽

Scid Mice ◽

Human Pancreatic Cancer ◽

Cell Counts ◽

Normal Tissue Toxicity

Abstract Background Epidermal growth factor receptors (EGFR) are overexpressed on > 90% of pancreatic cancers (PnCa) and represent an attractive target for the development of novel therapies, including radioimmunotherapy (RIT). Our aim was to study RIT of subcutaneous (s.c.) PANC-1 human PnCa xenografts in mice using the anti-EGFR monoclonal antibody, panitumumab labeled with Auger electron (AE)-emitting, 111In or β-particle emitting, 177Lu at amounts that were non-toxic to normal tissues. Results Panitumumab was conjugated to DOTA chelators for complexing 111In or 177Lu (panitumumab-DOTA-[111In]In and panitumumab-DOTA-[177Lu]Lu) or to a metal-chelating polymer (MCP) with multiple DOTA to bind 111In (panitumumab-MCP-[111In]In). Panitumumab-DOTA-[177Lu]Lu was more effective per MBq exposure at reducing the clonogenic survival in vitro of PANC-1 cells than panitumumab-DOTA-[111In]In or panitumumab-MCP-[111In]In. Panitumumab-DOTA-[177Lu]Lu caused the greatest density of DNA double-strand breaks (DSBs) in the nucleus measured by immunofluorescence for γ-H2AX. The absorbed dose in the nucleus was 3.9-fold higher for panitumumab-DOTA-[177Lu]Lu than panitumumab-DOTA-[111In]In and 7.7-fold greater than panitumumab-MCP-[111In]In. No normal tissue toxicity was observed in NOD/SCID mice injected intravenously (i.v.) with 10.0 MBq (10 μg; ~ 0.07 nmoles) of panitumumab-DOTA-[111In]In or panitumumab-MCP-[111In]In or in NRG mice injected i.v. with 6.0 MBq (10 μg; ~ 0.07 nmoles) of panitumumab-DOTA-[177Lu]Lu. There was no decrease in complete blood cell counts (CBC) or increased serum alanine aminotransferase (ALT) or creatinine (Cr) or decreased body weight. RIT inhibited the growth of PANC-1 tumours but a 5-fold greater total amount of panitumumab-DOTA-[111In]In or panitumumab-MCP-[111In]In (30 MBq; 30 μg; ~ 0.21 nmoles) administered in three fractionated amounts every three weeks was required to achieve greater or equivalent tumour growth inhibition, respectively, compared to a single amount of panitumumab-DOTA-[177Lu]Lu (6 MBq; 10 μg; ~ 0.07 nmoles). The tumour doubling time (TDT) for NOD/SCID mice with s.c. PANC-1 tumours treated with panitumumab-DOTA-[111In]In or panitumumab-MCP-[111In]In was 51.8 days and 28.1 days, respectively. Panitumumab was ineffective yielding a TDT of 15.3 days vs. 15.6 days for normal saline treated mice. RIT of NRG mice with s.c. PANC-1 tumours with 6.0 MBq (10 μg; ~ 0.07 nmoles) of panitumumab-DOTA-[177Lu]Lu increased the TDT to 20.9 days vs. 11.5 days for panitumumab and 9.1 days for normal saline. The absorbed doses in PANC-1 tumours were 8.8 ± 3.0 Gy and 2.6 ± 0.3 Gy for panitumumab-DOTA-[111In]In and panitumumab-MCP-[111In]In, respectively, and 11.6 ± 4.9 Gy for panitumumab-DOTA-[177Lu]Lu. Conclusion RIT with panitumumab labeled with Auger electron-emitting, 111In or β-particle-emitting, 177Lu inhibited the growth of s.c. PANC-1 tumours in NOD/SCID or NRG mice, at administered amounts that caused no normal tissue toxicity. We conclude that EGFR-targeted RIT is a promising approach to treatment of PnCa.

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Local Tumor Control and Normal Tissue Toxicity of Pulsed Low-Dose-Rate Radiation Therapy (PLRT) for Recurrent Lung Cancer: An In Vivo Study

International Journal of Radiation Oncology*Biology*Physics ◽

10.1016/j.ijrobp.2014.05.2278 ◽

2014 ◽

Vol 90 (1) ◽

pp. S788

Author(s):

P. Zhang ◽

B. Wang ◽

X. Chen ◽

D. Cvetkovic ◽

L. Chen ◽

...

Keyword(s):

Lung Cancer ◽

Radiation Therapy ◽

Normal Tissue ◽

Low Dose ◽

Local Tumor Control ◽

Tumor Control ◽

Local Tumor ◽

Low Dose Rate ◽

Normal Tissue Toxicity

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Neoadjuvant Radiotherapy-Related Wound Morbidity in Soft Tissue Sarcoma: Perspectives for Radioprotective Agents

Cancers ◽

10.3390/cancers12082258 ◽

2020 ◽

Vol 12 (8) ◽

pp. 2258

Author(s):

Cameron M. Callaghan ◽

M. M. Hasibuzzaman ◽

Samuel N. Rodman ◽

Jessica E. Goetz ◽

Kranti A. Mapuskar ◽

...

Keyword(s):

Wound Healing ◽

Soft Tissue ◽

Adjuvant Radiotherapy ◽

Normal Tissue ◽

Soft Tissue Sarcomas ◽

Limb Amputation ◽

Neoadjuvant Radiotherapy ◽

Normal Tissue Toxicity ◽

Radiation Induced ◽

Intensity Radiation

Historically, patients with localized soft tissue sarcomas (STS) of the extremities would undergo limb amputation. It was subsequently determined that the addition of radiation therapy (RT) delivered prior to (neoadjuvant) or after (adjuvant) a limb-sparing surgical resection yielded equivalent survival outcomes to amputation in appropriate patients. Generally, neoadjuvant radiation offers decreased volume and dose of high-intensity radiation to normal tissue and increased chance of achieving negative surgical margins—but also increases wound healing complications when compared to adjuvant radiotherapy. This review elaborates on the current neoadjuvant/adjuvant RT approaches, wound healing complications in STS, and the potential application of novel radioprotective agents to minimize radiation-induced normal tissue toxicity.

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MO-E-351-03: Functional MRI for Assessment of Treatment Response and Normal Tissue Toxicity

Medical Physics ◽

10.1118/1.2962399 ◽

2008 ◽

Vol 35 (6Part19) ◽

pp. 2877-2878

Author(s):

Y Cao

Keyword(s):

Treatment Response ◽

Functional Mri ◽

Normal Tissue ◽

Normal Tissue Toxicity

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TU-F-12A-09: GLCM Texture Analysis for Normal-Tissue Toxicity: A Prospective Ultrasound Study of Acute Toxicity in Breast-Cancer Radiotherapy

Medical Physics ◽

10.1118/1.4889364 ◽

2014 ◽

Vol 41 (6Part28) ◽

pp. 482-482

Author(s):

T Liu ◽

X Yang ◽

W Curran ◽

M Torres

Keyword(s):

Breast Cancer ◽

Acute Toxicity ◽

Texture Analysis ◽

Normal Tissue ◽

Cancer Radiotherapy ◽

Normal Tissue Toxicity ◽

Breast Cancer Radiotherapy ◽

Ultrasound Study

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The abscopal effect 67 years later: from a side story to center stage

British Journal of Radiology ◽

10.1259/bjr.20200042 ◽

2020 ◽

Vol 93 (1109) ◽

pp. 20200042 ◽

Cited By ~ 10

Author(s):

Sandra Demaria ◽

Silvia C Formenti

Keyword(s):

Normal Tissue ◽

Viral Infections ◽

Ionising Radiation ◽

Radiation Doses ◽

Abscopal Effect ◽

Rare Occurrence ◽

Cytotoxic Effects ◽

Normal Tissue Toxicity ◽

Canonical Pathways ◽

Effects Of Radiation

For over a century, ionising radiation has been used to treat cancer based on its cytotoxic effects on tumour cells. Technical progress has enabled more precise targeting of the tumour to reduce normal tissue toxicity while delivering higher radiation doses per fraction of treatment. In 1953, unexpected regression in lesions outside of the irradiated field were noted by an observant physician, RH Mole, who named such phenomenon “abscopal effect” from the Latin ab (position away from) and scopus (mark or target), in an article published in this journal. Clinical abscopal responses have been reported over the years but because of their very rare occurrence they could not be methodically studied, remaining akin to a curiosity. Nevertheless, their occurrence has ignited interest in studying the systemic effects of radiotherapy. Progress in dissecting the mechanisms that govern the function of the immune system in cancer has enabled to study the implication of immunity in the abscopal effect of radiation. It has become clear that ionising radiation activates canonical pathways of response to viral infections, and can stimulate antitumour immunity. These immune stimulatory effects of radiation have become clinically relevant in the current era of cancer immunotherapy, rendering abscopal responses in patients an attainable aim. Here, we will briefly review the parallel evolutions of two separate fields of medicine, radiation therapy and cancer immunology, and discuss their therapeutic partnership.

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Combining Radiotherapy and Immunotherapy in Lung Cancer: Can We Expect Limitations Due to Altered Normal Tissue Toxicity?

International Journal of Molecular Sciences ◽

10.3390/ijms20010024 ◽

2018 ◽

Vol 20 (1) ◽

pp. 24 ◽

Cited By ~ 22

Author(s):

Florian Wirsdörfer ◽

Simone de Leve ◽

Verena Jendrossek

Keyword(s):

Lung Cancer ◽

Clinical Trials ◽

Cancer Therapy ◽

Cancer Patients ◽

Cancer Biology ◽

Normal Tissue ◽

Radiation Treatment ◽

Current Knowledge ◽

Immune Checkpoint Blockade ◽

Normal Tissue Toxicity

In recent decades, technical advances in surgery and radiotherapy, as well as breakthroughs in the knowledge on cancer biology, have helped to substantially improve the standard of cancer care with respect to overall response rates, progression-free survival, and the quality of life of cancer patients. In this context, immunotherapy is thought to have revolutionized the standard of care for cancer patients in the long term. For example, immunotherapy approaches such as immune checkpoint blockade are currently increasingly being used in cancer treatment, either alone or in combination with chemotherapy or radiotherapy, and there is hope from the first clinical trials that the appropriate integration of immunotherapy into standard care will raise the success rates of cancer therapy to a new level. Nevertheless, successful cancer therapy remains a major challenge, particularly in tumors with either pronounced resistance to chemotherapy and radiation treatment, a high risk of normal tissue complications, or both, as in lung cancer. Chemotherapy, radiotherapy and immunotherapy have the capacity to evoke adverse effects in normal tissues when administered alone. However, therapy concepts are usually highly complex, and it is still not clear if combining immunotherapy with radio(chemo)therapy will increase the risk of normal tissue complications, in particular since normal tissue toxicity induced by chemotherapy and radiotherapy can involve immunologic processes. Unfortunately, no reliable biomarkers are available so far that are suited to predict the unique normal tissue sensitivity of a given patient to a given treatment. Consequently, clinical trials combining radiotherapy and immunotherapy are attracting major attention, not only regarding efficacy, but also with regard to safety. In the present review, we summarize the current knowledge of radiation-induced and immunotherapy-induced effects in tumor and normal tissue of the lung, and discuss the potential limitations of combined radio-immunotherapy in lung cancer with a focus on the suspected risk for enhanced acute and chronic normal tissue toxicity.

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