Background
Thymic carcinomas (TCs) are aggressive mediastinal malignant tumors with an annual incidence of 1.3–3.2 per million [
1,
2]. Patients with early-stage TCs often choose to undergo complete surgical resection and postoperative adjuvant radiotherapy. Paclitaxel combined with carboplatin is the recommended first-line treatment for patients with according to the National Comprehensive Cancer Network guideline with an overall response rate (ORR) of 22–36%. Unfortunately, advanced TCs show a limited response to chemotherapy and patients with TCs lack an effective second-line regimen after disease progression. Chemotherapy has shown a median progress-free survival time (mPFS) of 4.3–7.6 months as a second-line therapy in patients with recurrent TCs according to several prospective phase 2 studies [
3‐
6]. In recent years, targeted drugs and immune checkpoint inhibitors (ICIs) have made some progress for the treatment of advanced thymic carcinomas. For previously treated TCs patients, the mPFS and ORR of ICIs monotherapy (pembrolizumab and nivolumab) were 3.8–6.1 months and 0–22.5%, respectively [
7‐
9]. Clinical studies on second- and posterior treatment options for TCs are numerous, although most are limited to small samples and evidence from randomized controlled trial is lacking. As such, for patients with TCs who have progressed after first-line platinum-containing chemotherapy, standard second- or post-line treatment regimens have not been confirmed.
Over recent years, the efficacy of angiogenesis therapy in advanced non-small cell lung cancer, soft tissue sarcoma, and radioactive iodine-refractory differentiated thyroid cancer has been recognized. Clinical studies of antiangiogenic drugs in the treatment of metastatic TCs are gaining attention. For example, lenvatinib, sunitinib, bevacizumab and regorafenib have all showed some antitumor activity in patients with previously treated TCs [
10‐
15]. Lenvatinib is known to exhibit the highest ORR of 38% as the second-line treatment in metastatic TCs patients [
10].
Vascular endothelial growth factor receptor-2 (VEGFR2) and platelet-derived growth factor receptor-α (PDGFR-α) are known to be activated and involved in the growth and progression of TCs [
16‐
19]. However, evidence on the efficacy of anlotinib and apatinib in the treatment of advanced TC is limited. Anlotinib is a newly developed oral small-molecule tyrosine kinase inhibitor (TKI) that targets VEGFR1, VEGFR2/KDR, VEGFR3, c-Kit, PDGFR-α, and the fibroblast growth factor receptor (FGFR1, FGFR2, and FGFR3). Furthermore, anlotinib can inhibit both tumor angiogenesis and tumor cell proliferation [
20,
21]. Apatinib exerts its antigenic effects by inhibiting VEGFR-induced proliferation and migration of endothelial cells via the selectively targeting of VEGFR2 [
22].
Based on this background, we explored the efficacy and toxicity of small molecule antiangiogenic drugs in previously treated patients with advanced TCs in the real-word.
Methods
Patients
All patient information was obtained from the electronic medical records system of Zhejiang Cancer Hospital (Hangzhou, Zhejiang). Patients with pathologically documented metastatic TCs (stage IVA or IVB defined by the Masaoka-Koga classification) after failure of first-line or multiline chemotherapy who used small molecule antiangiogenic drugs in the next were included in this study from January 2010 to December 2021. The inclusion criteria were as follows: (1) Eastern Cooperative Oncology Group (ECOG) performance status 0 or 1, (2) at least one measurable target lesion defined by the Response Evaluation Criteria in Solid Tumors (RECIST) version 1.1 and (3) received at least two cycles of small molecule antiangiogenic therapy after progression on a first-line platinum-based chemotherapy. The exclusion criteria were: (1) patients received immunotherapy or other targeted agents other than small molecule antiangiogenic drugs, (2) patients had an active autoimmune disease, and (3) patients had malignant tumors of other sites. Recurrence or metastases were performed evaluated by chest computed tomography (CT) scan, abdominal brain CT, or bone scans.
The study protocol was approved by the Institutional Ethics Committee at Zhejiang Cancer Hospital (No. IRB-2022-62). Individual patient consent was not required for this study.
Responses assessments
Patients received oral apatinib 250–500 mg per day or oral anlotinib 12 mg per day for 2 weeks, with 1 week off; each cycle was 3 weeks in length. Tumor responses were assessed every two cycles or evaluated early when significant signs of progression appeared. Objective tumor responses were according to RECIST 1.1, and include complete response (CR), partial response (PR), stable disease (SD), and progressive disease (PD). Treatment related adverse events (AEs) grade as assessed by the National Cancer Institute Common Terminology Criteria for Adverse Events (CTCAE) version 5.0.
Statistical analysis
Data analyses were conducted using SPSS version 25 (SPSS Inc., Chicago, IL, USA) software. T test was used for normally distributed variables such as age between groups. The non-parametric rank sum test was used for continuous variables between groups that were not normally distributed. Other categorical variables were compared using Fisher’s exact Chi-squared test. P < 0.05 was considered significant. Survival analysis was calculated using the Kaplan-Meier method. PFS encompassed the time from the first cycle of antiangiogenic drugs therapy to documented progression or death from any cause. Overall survival (OS) was defined as the time diagnosed with advanced thymic carcinoma to death from any cause or last follow-up. COX regression was used for the univariate analysis of PFS and OS and significant variables (P < 0.05) were included in subsequent multivariate analysis. The median follow-up period was 46.0 months (95% confidence interval [CI], 33.0–59.0 months, adverse Kaplan-Meier estimated) and the last follow-up was the 17th of April 2022.
Discussion
To the best of our knowledge, this is the first real-world retrospective study of small molecule antiangiogenic drugs for previously treated thymic carcinoma in China. This research involved the largest sample size of small molecule antiangiogenic drugs for advanced TCs. Our analysis showed that apatinib and anlotinib exhibited considerable antitumor activity and durable responses in advanced TCs.
We summarized the phase II studies of small molecule antiangiogenic drugs in advanced thymic carcinomas (Table
4). Four phase II studies have explored the efficacy of antiangiogenic drugs (lenvatinib, sunitinib, apatinib, and regorafenib) for the treatment of advanced TCs. The
National Comprehensive Cancer Network (NCCN) Guidelines Version 2.2022 Thymomas and Thymic Carcinomas recommended sunitinib with an ORR of 26.0% as the second-line treatment regimen for advanced TCs [
11]. Another phase II trial of lenvatinib for 42 patients with advanced TCs, reported the best ORR of 38.0% (95% CI, 25.6–52.0,
p < 0.0001), a mPFS of 9.3 (95% CI, 7.7–13.9) months, and a DCR of 95.0%. Similarly, the most common grade 3 AEs were hypertension (64.0%) and hand-foot syndrome (7.0%). Song et al. [
23] previously evaluated the efficacy of apatinib in the treatment of advanced TCs, with an ORR, DCR, mPFS and mOS of 20.0 and 73.0%, 6.1 months (95%CI, 2.6–9.6 months) and 24.0 months (95%CI, 16.1–not evaluable (NE) months), respectively. Another phase II study [
15] explored the efficacy of regorafenib monotherapy in eight patients with TCs as the second-line regimen. These authors reported a mPFS of 9.2 months (95% CI, 0.9–34.0 months) and a mOS of 20.1 months (95% CI, 0.9–NE) months, although the ORR was 0.0% according to the RECIST criteria.
Table 4
Phase II study of small molecule antiangiogenic agents in advanced thymic carcinomas
| 2015 | Phase II | Sunitinib | 25TC | 7.2 | NA | 26.0% |
| 2020 | Phase II | lenvatinib | 42TC | 9.3 | NA | 38.0% |
| 2022 | Phase II | Apatinib | 15TC | 6.1 | 24.0 | 20.0% |
| 2022 | Phase II | Regorafenib | 8TC | 9.2 | 20.1 | 0.0% |
In addition, Yudong et al. [
24] (2018) reported a case of advanced thymic squamous cell carcinoma with EGFR exon 20 insertion that was effectively treated with apatinib after the failure of multiple lines of chemotherapy. The patient had received a partial response after 5 months of treatment and the PFS was 10.0 months. Similarly, a patient with advanced thymic squamous carcinoma with EGFR 20 exon insertion was successfully treated with apatinib and anlotinib after failure of previous multiline therapy [
25]. This study showed that after reaching a PFS of 13.0 months with apatinib treatment, the patient was switched to anlotinib due to adverse effects. The PFS of anlotinib was 23.0 months and the OS was 6 years. After treatment with apatinib failed, anlotinib was able to control the patient’s mediastinal mass and all adverse effects were tolerated. He et al. [
26] (2018) also reported a case of partial response following daily treatments with apatinib for advanced TC; the PFS was 6.3 months and drug-related toxicities were tolerable.
In contrast with previous studies, our present research included two small molecule TKI drugs for the treatment of TCs. Certainly, the ORR of this study was consistent with that of the four phase II studies. We observed a mOS of 47.0 (95%CI, 35.4–58.6 months) after a median follow-up of 46 months and there were eight (47.1%) surviving patients at the last follow-up date. In addition, we did not identify any significant difference in terms of efficacy between anlotinib and apatinib. Head-to-head studies of anlotinib and apatinib in advanced thymic carcinomas are now expected.
VEGF is involved in the development of normal blood vessel networks in the thymus [
16]. Several previous studies have shown that VEGFR1 and VEGFR2 are highly expressed in thymic carcinomas. Angiopoietin 1 and VEGF are known to be the most up-regulated growth factors in TCs [
17,
18,
27].
Our real-world data also reported the efficacy of antiangiogenic drugs for the treatment of advanced TCs. Consequently, small molecule angiogenesis therapy may represent a new treatment option for recurrent or metastatic advanced thymic carcinoma patients. TKIs have been observed to alter the tumor microenvironment by inducing immune microenvironment remodeling [
28,
29]. Small molecule antiangiogenic agents combined with ICIs have shown good efficacy for a variety of solid tumors [
30,
31]. Thus, novel combinations of small molecule antiangiogenic drugs with ICIs in patient with recurrent TCs need to be explored further. For example, a clinical trial of pembrolizumab in combination with sunitinib for advanced TCs (NCT03463460) is ongoing.
There are some limitations to our study that need to be considered. Firstly, this was a single-center, retrospective study and therefore retrospective nature of this study could have influenced some of the results. Second, only a limited number of cases were included in our study due to the fact that thymic tumors are relatively rare. Finally, this study was also limited by the small sample size in subgroup analysis.
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