The Safety and Treatment Response of Combination Therapy of Radioimmunotherapy and Radiofrequency Ablation for Solid Tumor: A Study In Vivo

Shu-Guang Zheng; Hui-Xiong Xu; Le-Hang Guo; Lin-Na Liu; Feng Lu

doi:10.1371/journal.pone.0096539

Abstract

Objection

To investigate the safety and treatment response of radioimmunotherapy (RIT) in combination with radiofrequency ablation (RFA) for the treatment of VX₂ tumor on rabbit.

Materials and Methods

A total of 36 rabbits bearing VX₂ tumor on the thigh were randomly assigned into 3 groups (group I: 1–2 cm; group II: 2–3 cm; group III: 3–4 cm) and 4 subgroups (A: as control, just puncture the tumor using the RFA electrode without power output; B: RFA alone; C: ¹³¹I-chTNT intratumoral injection alone; D: RFA+¹³¹I-chTNT intratumoral injection 3 days later). The variation of blood assay, weight and survival among different groups and subgroups were used to assess the treatment safety. Ultrasound (US) was used to monitor and assess the tumor response after treatment.

Results

According to the results of the weight and the blood assay among different groups, subgroups, and at two time points (one day before and the 16th day after treatment), no damages to the liver, kidney function and myelosuppression resulting from the treatment were found. No significant differences in survivals among the four subgroups (p = 0.087) were found. In addition, ¹³¹I-chTNT did not show significant inhibition effect on VX₂ tumor progression according to US measurements.

Conclusion

¹³¹I-chTNT intratumoral injection alone or in combination with RFA is relatively safe for rabbit without significant toxicity and shows no significant effect on the survival. The treatment response is not as satisfactory as anticipated.

Citation: Zheng S-G, Xu H-X, Guo L-H, Liu L-N, Lu F (2014) The Safety and Treatment Response of Combination Therapy of Radioimmunotherapy and Radiofrequency Ablation for Solid Tumor: A Study In Vivo. PLoS ONE 9(5): e96539. https://doi.org/10.1371/journal.pone.0096539

Editor: David Loeb, Johns Hopkins University, United States of America

Received: January 3, 2014; Accepted: April 8, 2014; Published: May 2, 2014

Copyright: © 2014 Zheng et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Funding: Supported by National Scientific Foundation Committee of China, No. 30970837, 81371570, 81301229. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Competing interests: The authors have declared that no competing interests exist.

Introduction

Radioimmunotherapy (RIT) is a powerful and attractive tool for the treatment of local and/or diffuse tumors with radiation [1], [2]. The use of antibody conjugated radionuclides firstly started in the early 1950s [3]. Recently, the major advance in RIT is the treatment of hematological malignances that the FDA has approved use of ⁹⁰Y ibritumomab tiuxetan (Zevalin) and ¹³¹I tositumomab (Bexxar) in treating non-Hodgkins’ lymphoma (NHL) [4]–[7].

However, for solid tumors, RIT is still challenging and only few clinical trials have gone beyond Phase II, which stimulates more researchers to explore this issue [1], [8]. Song et al [4] proposed that two therapeutic components: radiation delivery and antibody action upon binding were the main contribution to kill cancer cells and to enhance the overall tumor response; Huang et al [9] also mentioned that therapeutic efficacy of RIT to solid tumor was limited by the inadequate delivery and penetration of RIT agents into solid tumor. Thus, most of recent studies have focused on how to improve the tumor uptake [10]. Whether the higher targeting concentration of RIT agents will acquire better response for solid tumors is still controversial.

In a previous study on rabbit bearing VX₂ tumor, RFA before intratumoral injection of ¹³¹I-chTNT dramatically improving the targeting concentration (the tumor to normal tissue ratio [T/NT] from 7.63±5.61 to 55.45±41.83) had been demonstrated [11]. The VX₂ tumor is an anaplastic squamous cell carcinoma derived from a virus-induced papilloma in the wild rabbit, but appears as a carcinoma in the domestic species. Tumor necrosis therapy (TNT) uses degenerating tumor cells and necrotic regions of tumors as targets for RIT. ¹³¹I-chTNT is an 131-iodine radiolabeled chimeric monoclonal antibody (MAb) targeted against intracellular DNA exposed in necrotic and degenerating regions of malignant solid tumors, which has shown some promising applications in some clinical trials for treatment of lung cancer, glioblastoma, colorectal carcinoma, and other malignant solid tumors [8], [11]–[13]. Radiofrequency ablation (RFA) is also a validated therapeutic modality for the treatment of some solid tumors of the whole body [14]–[17]. Then as far as intratumoral injection of ¹³¹I-chTNT in combination with RFA was concerned, whether therapeutic efficacy could be improved along with the improvement of RIT agent targeting concentration and how about their safety are worth to be further investigated. On the basis of the above-mentioned, this study was aimed to assess the treatment efficacy and safety of intratumoral injection of ¹³¹I-chTNT in combination with RFA for the treatment of VX₂ tumor on rabbit.

Materials and Methods

Preparation of the Animal Model

All animal experiments were approved by animal research ethic committee of Sun Yat-sen University, China. During all the procedures, animal welfare was carried out according to the ARRIVE (Animal Research: Reporting of In Vivo Experiments) Guidelines. A total of 36 New Zealand white rabbits weighting 2.33±0.32 kg (range, 1.9–2.9 kg) and bearing VX₂ tumor on the thigh were enrolled in this study. The rabbits were purchased from the laboratory animal center of Guangdong and the VX₂ tumor was obtained from Laboratory Animal Center, Sun Yat-sen University, China.

All the rabbits were randomly and equally assigned into 3 groups (12 rabbits in each group). When the VX₂ tumor grew up to the anticipated size (group I: 1–2 cm, group II: 2–3 cm, group III: 3–4 cm), each group was further divided into 4 subgroups (3 rabbits in each subgroup) randomly to receive treatments as follows:

Subgroup A: as control, just puncture the tumor using the RFA electrode without power output;
Subgroup B: RFA alone;
Subgroup C: 131I-chTNT intratumoral injection alone;
Subgroup D: RFA+131I-chTNT intratumoral injection 3 days later.

Treatments

All rabbits received a solution of potassium iodine orally, beginning from 3 days before treatment and lasting to the 15th day after treatment, to block uptake of free iodine-131 by their thyroid. Before treatment, the rabbits were anesthetized by injection with 3% pentobarbital solution (1 mL/kg) via ear vein and were fixed on the bed in left lateral decubitus; the thighs of the rabbits were shaved and prepared with povidone iodine. US machine (M-Turbo Ultrasound system, Sonosite Inc, Bothell, Washington, USA) equipped with a transducer with frequency of 13-6 MHz was performed in the experiments for puncture guidance. All treatments were performed under sterile condition.

RFA

RFA procedures were performed using a Cool-tip system (Valleylab, Boulder, Colo, USA), which consists of an RF generator with a maximum power of 200 W, a 20 cm-long 17-gauge internally cooled electrode with a 3 cm active tip, and a dispersive ground pad was attached on the shaved back of the rabbits. Under the guidance of US, the RFA electrode was inserted into the VX₂ tumor along the longest diameter with energy output of 50 w for 3 min.

¹³¹I-chTNT

¹³¹I-chTNT (Vivatuxin, Shanghai Medipharm Biotech Co. Ltd, Shanghai, China) is a radiolabeled recombinant human-mouse chimeric TNT (ch-TNT) antibody. The purified ch-TNT antibody with purity of at least 98% is radiolabeled with Na¹³¹I, which has a radioactive range of 2.2 mm in the tissue and a half-life of 8 days. The purity of ¹³¹I-chTNT is over 95% with a specific radioactivity of 10 mCi/mL (370 MBq/mL).

¹³¹I-chTNT was injected into the VX₂ tumor by using a 22-gauge fine core needle with a recommended dose of 1.4 mCi/cm³ VX₂ tumor from the manufacturer. This dose was calculated according to the reported formula for dose translation based on the body surface area by Reagan-Shaw et al [18]. The US guidance made sure of the accurate placement of the needle at multiple sites (0, 3, 6, 9 o’clock direction) and simultaneously monitored the ¹³¹I-chTNT injection and observed its distribution in the VX₂ tumor. After injection of ¹³¹I-chTNT, 0.5 mL normal saline was used to flush the needle. The puncture site was then gently compressed using alcoholic cotton gauze for 2 min to avoid leakage of ¹³¹I-chTNT or bleeding after removal of the needle.

SPECT/CT Fusion Imaging

At the first day after ¹³¹I-chTNT injection, the rabbits (in the subgroup C and D) underwent SPECT/CT scanning for acquiring fusion image to observe the distribution of ¹³¹I-chTNT. The acquisition parameters of SPECT/CT (Symbia T2 SPECT/CT system, Siemens Munich, Germany) were used as follows: zoom 1.5, a 128×128 matrix with a pixel acquisition, the fusion CT acquisition used full-circle rotation, 130 kV, 35 mAs, and 5-mm slices.

Safety and Survival

The treatment safety for the rabbit was assessed mainly on the basis of blood assay, weight and survival. At two time points (1 day before and the 16th day after treatment), the blood samples were drawn from the ear artery of the rabbits for testing the count of blood cell (CBC) (including: white blood cell, WBC; red blood cell, RBC; hemoglobin, HB; platelet, PLT), liver function (including: alkaline phosphates, ALP; aspartate transaminase, AST; alanine aminotransferase, ALT; total protein, TP; albumin, ALB;) and kidney function (including: blood urea nitrogen, BUN; creatinine, Cr). Simultaneously, all rabbits were weighed. After treatment, all rabbits were raised and checked twice every day for observing the survival. The humane endpoint was defined by >50% decrease in food intake and >20% loss in body weight. Then they were humanely euthanized by injection of overdose 3% pentobarbital solution (>3 mL/kg) via ear vein.

Treatment Response and Progression after Treatment

During the follow-up period after treatment, US was performed by two operators independently for measuring the three greatest dimensions (x, y, z) at 3 days interval until the 15th day. Meanwhile the tumor volumes (TV) were calculated according to the following formula:π•x•y•z/6. The mean TV was used for evaluating the treatment response.

On the basis of the TV, The tumor volume growth rate (TVGR) at n day and the tumor volume growth rate at each interval (TVGRI) were calculated based on the following equations:V_n and V_initial were the tumor volume of each group measured at n day and start of the treatment respectively.

Finally, on the basis of the TV, the tumor growth curve was drawn. The treatment response and tumor progression were evaluated by comparing the TV, TVGR and TVGRI.

Statistical Analysis

Continuous data were expressed as mean ± standard deviation. Multiple comparisons were performed using univariate/repeated measures analysis of variance (ANOVA) with Bonferroni-test. Kaplan-Meier survival curves for overall survival were generated, and the log-rank test was used to identify the difference between the subgroups. The level of statistical significance was set at P<0.05. SPSS software (version 16.0, SPSS Inc., Chicago, IL, USA) was used to perform the statistical analysis.

Results

During the whole experimental procedure, US was used to measure the VX₂ tumor size (Figure 1. A, B, C), guide percutaneous RFA electrode insertion and monitor the treatment procedure (Figure 1. D, E, F).

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Figure 1. The ultrasound images of VX₂ tumor and puncturing guidance.

A, B, C: a VX₂ tumor on ultrasound (US) at 0, 6th and 12th day after treatment, respectively; D: ¹³¹I-chTNT intratumoral injection; E: after ¹³¹I-chTNT intratumoral injection; F: radiofrequency ablation (RFA). Thin arrow: the VX₂ tumor; thick arrow: PTC needle (D) or RFA electrode (F).

https://doi.org/10.1371/journal.pone.0096539.g001

Until the 16th day after the treatment, no severe complications or death were encountered. On SPECT/CT fusion image at the first day after intratumoral injection,¹³¹I-chTNT was observed overlapping the VX₂ tumor with a high concentration (Figure 2).

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Figure 2. The SPECT/CT fusion images.

The fusion images show the injected ¹³¹I-chTNT overlaps with the tumor.

https://doi.org/10.1371/journal.pone.0096539.g002

The results of the weight and the blood assay including CBC, liver and kidney function at two time-points (one day before and the 16th day after treatment) were listed in Table 1. Based on the analysis results of the above-mentioned parameters, no significant differences were found among different groups (all p>0.05); No significant differences were found among different subgroups (all p>0.05), except for BUN, Cr, ALP and ALB (all p<0.05); Additionally, no significant differences were found between the two time-points (all p>0.05), except for ALB, WBC and PLT(all p<0.05). Thus no damages to the liver, kidney function and myelosuppression resulting from the treatment were found.

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Table 1. The results of the weight and the blood assay of rabbit before and after treatment.

https://doi.org/10.1371/journal.pone.0096539.t001

According to US measurement results during the follow-up from the treatment beginning to the 15th day after treatment, the TV, TVGR and TVGRI were calculated and listed in Table 2 and Table 3, respectively. According to the analysis results, all data were normally distributed and met the homogeneity of variance. Accordingly, the growth curve of the tumor in each group was drawn (Figure 3). Regarding TVGR and TVGRI, no significant differences were found among different groups (all p>0.05); but both parameters between subgroup A and B, A and D, B and C, and C and D, showed significant difference (all p<0.05). Obviously, unlike RFA, ¹³¹I-chTNT had no significant inhibition effect on VX₂ tumor progression.

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Figure 3. The growth curves of the tumors after treatment in group I, II, III.

Multiple comparisons among different subgroups (Bonferroni-test).

https://doi.org/10.1371/journal.pone.0096539.g003

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Table 2. The tumor volumes (TVs) of VX₂ tumors during the follow-up.

https://doi.org/10.1371/journal.pone.0096539.t002

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Table 3. The tumor volume growth rate (TVGR) and the tumor volume growth rate at each interval (TVGRI) of VX₂ tumors during the follow-up.

https://doi.org/10.1371/journal.pone.0096539.t003

After treatment, all rabbits were followed up until the 120th day and finally were humanely euthanized when they met the above-mentioned criteria of the endpoint, except for 2 rabbits in subgroup B of group I. Subsequently, the survival curves were drawn on the basis of the survivals of the rabbits (Figure 4). The log-rank test revealed that there was no significant difference among the four subgroups (p = 0.087).

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Figure 4. The survival curves of the rabbits in four subgroups.

Multiple comparisons among different subgroups (p = 0.087, log-rank test).

https://doi.org/10.1371/journal.pone.0096539.g004

Discussion

Enhancing the overall response/survival and decreasing the toxicity are always the main pursues of RIT for treatment of various solid tumors. In the past decades, much effort has been focused on the development of the best targeting vector, choosing the most appropriate isotope, and finding the suitable administration procedure [1], [2], [4], [10], [19]–[22].

It is reported that multiple barriers to delivery still exist which prevent effective immunotherapy for solid tumors in vivo, such as hemodilution, renal excretion, neutralization of free antibodies and block of vascular endothelial cell, physical decay, short radiation range and duration, and so on [1], [2], [4], [9], [19]. Hence a series of antibodies with higher active targeting ability have been explored for the application of RIT; meanwhile many strategies including the pre-targeting technique, administration via tumorous supply artery, and intratumoral injection, have been employed [1], [2], [9], [21]–[24].

Recently, it is proposed that RIT could be combined with other treatments to enhance the efficacy [1], [2], [24]–[28]. For instance, US-guided percutaneous local treatments are playing increasingly important roles for a variety of solid tumors. Barbet et.al [20] mentioned that the loco-regional route is preferable for the radionuclides when targeted by antibodies because using the intravenous route always results in significant radionuclide decay before the antibody has reached its target. Therefore, US guided ¹³¹I-chTNT intratumoral injection in combination with RFA was performed in this study.

Theoretically, a higher targeting concentration of RIT agents, will achieve a better treatment response and a less toxicity. Chen et al [8] reported a phase II clinical trial conducted in China on 107 patients with advanced lung cancer. ¹³¹I-chTNT (0.8mCi/kg) was administered by intravenous injection at 2–4 weeks interval (n = 62) and intratumoral injection (n = 45). At 10 weeks post-treatment, in spite of some mild side effects and reversible bone marrow suppression, the intratumoral injection (less hematologic toxicity) was proven to be safer than intravenous injection. The overall response rates were up to 35.5%. Unfortunately, no evidence of benefit to the overall survival was documented [8].

In this study, US guided direct ¹³¹I-chTNT intratumoral injection was used to avoid the hemodilution and RFA was performed in advance to increase the targeting site of ¹³¹I-chTNT. The fused SPECT/CT image on the first day after treatment also proved a high targeting concentration of 131-iodine. No significant differences regarding the hematologic toxicity of ¹³¹I-chTNT, as well as weight, liver and kidney function, were found among different subgroups. Furthermore, the post-treatment survival among different subgroups also did not show significant difference. That is to say, ¹³¹I-chTNT with or without RFA was safe enough for rabbit.

However, the treatment response of VX₂ tumor was not as expected as that of the lung cancer [8]. As mentioned above, RFA is a validated therapeutic modality for the treatment of some solid tumors. On the other hand, ¹³¹I-chTNT was not found effective for the treatment of VX₂ tumor, whether used alone (all Subgroup A vs. C, p>0.05) or combined with RFA (all Subgroup B vs. D, p>0.05), despite that RFA in advance can dramatically improve the targeting concentration of ¹³¹I-chTNT after intratumoral injection [11]. Thus improving the targeting concentration of RIT agents alone seems inadequate for RIT of some kinds of solid tumors. In the case of RIT, as Navarro-Teulon et al [1] have mentioned, solid tumors are more radio-resistant than hematological malignancies. Hannaoka et al [29] also concluded that the therapeutic efficacy of RIT seems largely dependent on the tumor radiosensitivity. Therefore the radiosensitivity should be regarded as the fundamental element responsible for treatment response of solid tumors, besides the targeting MAbs, isotopes and administration modalities. Thus, further studies should be focused on how to enhance the tumor response.

There were some limitations in this study as follows: firstly, just VX₂ tumor model on rabbits was used without other tumor model as comparison. Furthermore, no various dose of ¹³¹I-chTNT were performed to investigate the VX₂ tumor response and the sensitive dose. Additionally, although no significant differences in survival were found, the Kaplan-Meier survival analysis showed that the subgroup that received RFA only differed quite substantially from the others, possibly due to the hematological toxicity in the RIT subgroups. Finally, the blood assay was just performed at two time points without further comparison at longer time point.

Conclusion

In summary, ¹³¹I-chTNT intratumoral injection alone or in combination with RFA is relatively safe for rabbit without significant toxicity and shows no significant effect on the survival. In addition, the treatment response for the combined therapy was not as satisfactory as anticipated.

Author Contributions

Conceived and designed the experiments: HXX. Performed the experiments: SGZ LHG LNL FL. Analyzed the data: SGZ. Contributed reagents/materials/analysis tools: SGZ. Wrote the paper: SGZ HXX.

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Figures

Abstract

Objection

Materials and Methods

Results

Conclusion

Introduction

Materials and Methods

Preparation of the Animal Model

Treatments

RFA

131I-chTNT

SPECT/CT Fusion Imaging

Safety and Survival

Treatment Response and Progression after Treatment

Statistical Analysis

Results

Discussion

Conclusion

Author Contributions

References

¹³¹I-chTNT