Oncogene addiction and radiation oncology: effect of radiotherapy with photons and carbon ions in ALK-EML4 translocated NSCLC

Lung cancer is the leading cause of cancer mortality worldwide, and NSCLC comprises about 80% of lung cancer cases. Most patients are diagnosed with non-resectable diseases and approximately 1/3 present with locally advanced diseases (stage III) i.e., the tumor may exceed the structures of the lung itself and/or have spread to ipsilateral mediastinal and/or subcarinal lymph nodes, but no clinical evidence for distant metastasis is found [1]. Radiochemotherapy is an integral component of the multimodal treatment for these locally advanced patients. Despite improvements in radiotherapy delivery, different chemotherapy combination and schemes, the median survival in this relatively heterogenous collective population is ~ 21 months with 3 years survival rates of ~ 30% [2‐8].

The chromosomal rearrangement between ALK and EML4 was first reported by Soda et al. from a resected specimen of a male lung adenocarcinoma patient [9]. Between 3% to 7% of NSCL tumors harbor the EML4-ALK fusion [10, 11]. It is predominantly detected in adenocarcinomas of light smokers (< 10 packs per year) or non-smokers at a younger age, and is independent of epidermal growth factor receptor (EGFR) or KRAS mutations [12]. The EML4-ALK fusion protein leads to an aberrant activation of the ALK tyrosine kinase and its related downstream signaling [13]. A number of interconnected pathways are involved in ALK downstream signaling among which the MAP Kinase pathways including Ras- ERK and phosphoinositide 3-kinase (PI3K)-Akt are best characterized [14]. Activation of ALK-mediated signaling pathways plays a key role in tumorigenic transformation of cells by promoting cell growth and inhibiting apoptosis, irrespective of the originating organ [15, 16]. Soda et al. have shown that cells overexpressing EML4-ALK are able to generate subcutaneous or lung orthotopic tumors in a nude mouse model [9, 17]. Another chromosomal translocation between the nucleophosmin (NPM) gene on chromosome 5q35 and ALK gene on 2p23 is expressed in 60%–70% of anaplastic large cell lymphoma (ALCLs) [13, 18, 19].

Based on the discoveries of ALK as an important oncogene and the encoded fusion protein in development of different cancers, a search for small molecular ALK-tyrosine kinase inhibitors (TKIs) identified Crizotinib (PF-02341066) as the first in class compound receiving FDA-approval for treatment of ALK-positive advanced lung cancer in 2011 [20]. However, Crizotinib was originally identified in a screening program searching for a c-Met receptor tyrosine kinase inhibitor (RTKi). Accordingly, Crizotinib is not considered a specific ALK-inhibitor (with a half maximal inhibitory concentration, IC₅₀: 24 nM) and more potently inhibits other kinases such as c-Met (IC₅₀: 11 nM) [21] and ROS1 (IC ₅₀: 1.7 nM) [10]. Moreover, a gatekeeper mutation in the active kinase domain (L1196 M) renders ALK-positive lung cancer cells resistant to Crizotinib therapy [22]. In contrast, ALK-positive NSCLC cells harboring this gatekeeper mutation remain highly sensitive to second generation ALK-inhibitors such as TAE684 [22, 23].

TAE684 is a potent and selective ALK-inhibitor with a reported IC₅₀ of ~ 3 nM in ALK positive cell lines [24]. It was first reported to block the growth of ALCL-derived and ALK-dependent cell lines with IC₅₀ values between 2 and 10 nM [25]. The inhibitory effects were also observed in NSCLC cell lines with IC₅₀ values between 15 and 50 nM [23]. TAE684 was shown to induce apoptosis and cell cycle arrest via rapid and sustained inhibition of NPM-ALK phosphorylation and its downstream effectors including ERK, Akt and STAT3 and/or STAT5b [25].

Currently, ALK-inhibitors are approved only for advanced NSCLC. The translation of ALK-inhibitors in locally advanced NSCLC patients with EML4-ALK fusion will largely depend on a better understanding of the effects elicited by this novel class of drugs in combination with radiotherapy. Therefore, we aimed to explore the interaction of radiotherapy and ALK-inhibition by TAE684 in tumor cell lines with and without ALK-fusion. This is, to our knowledge the first report on beneficial effects of this combination in ALK-positive tumors. It further supports the concept of targeting oncogene addiction combined with radiotherapy, preferably with carbon ions, investigated at the German Research Foundation (DFG) “clinical research group heavy ion therapy (KFO-214)” within the project TP5 “Heavy Ions in Lung Cancer”.

Here we report on beneficial effects of combined ALK-inhibition and radiotherapy in NSCLC with EML4-ALK-fusion leading to a constitutive activation of ALK-signaling. Inhibition of ALK-signaling by TAE684 potently and selectively augmented antiproliferative and pro-apoptotic effects of irradiation in ALK-positive tumors. This combination further elicited synergistic effects in reducing the clonogenic survival of ALK-positive H3122 cells. In contrast to ALK-positive H3122 tumor cells, addition of TAE684 does not affect the antiproliferative effect of radiotherapy in two other NSCLC lacking ALK-activation. While the clonogenic survival was moderately reduced by addition of TAE684 to radiotherapy in A549 cells, TAE684 exerted a radioprotective effect in LLC cells as shown by clonogenic survival assays. This data suggests a narrowed indication for combined radiotherapy and ALK-inhibition only in NSCL tumors with aberrant ALK-activation. In contrast to conventional x-ray irradiation, TAE684 moderately sensitized LLC cells (SER: 1.27) when combined with carbon ion irradiation. Hence, radiation quality specific differences may exist in NSCLC response to ALK-inhibitors that warrants further investigation. This is in line with recently reported data on differential phosphoproteome response of NSCLC cells to conventional radiotherapy vs. proton and carbon irradiation [29]. Together with data of enhanced eradication of otherwise radioresistant tumor stem cells by carbon ions, these data indicate further exploration of distinct radiobiological features of different radiation qualities [30]. The potent sensitizing effects of TAE684 on carbon ions observed in ALK-positive H3122 cells (SER: 1.61) suggest further evaluation of this combination in the emerging field of high-LET particle therapy. These data are in complete alignment we recently reported data for combined crizotinib and radiotherapy in NSCLC based on tumor ALK status as schematically summarized in Fig. 5 [30].

High-precision irradiation with carbon ions has shown promising clinical outcomes in NSCLC [31, 32]. Addition of ALK-inhibitors in ALK-positive NSCLC may therefore augment local control effects of radiotherapy and in parallel provide a systemic therapy option to prevent distant tumor growth as the key pattern of therapy failure. Promising data on beneficial effects of combined ALK-inhibition and carbon ion irradiation reported in this study suggest further validation of this concept in preclinical in-vivo tumor models.

TAE684 is a potent small-molecule inhibitor of ALK activity that was shown to block the growth of ALK-dependent cells [25]. In contrast to the FDA/EMA approved, less specific ALK-inhibitor Crizotinib, the selectivity of TAE684 for ALK inhibition was demonstrated across a panel of 22 Kinases and between 100 to 1000 fold higher concentrations of TAE684 was required to inhibit other tyrosine kinases [25]. It was initially identified to inhibit proliferation of ALCLs that harbor the t (2; 5) (p23; q35) chromosomal translocation between ALK and NPM. NPM-ALK is a potent oncogene, possessing strong transforming ability in a wide array of different cell types in vitro and hematopoietic cell lines such as the myeloid line 32Dcl3 [33]. The 80-kD fusion protein is an oncogenic tyrosine kinase that activates downstream signaling pathways related to mitogenic, antiapoptotic and possibly DNA repair capabilities such as PI3K-Akt and JAK-STAT pathways [34‐38]. Further studies are needed to identify the relevance of different proposed ALK-downstream signaling pathways in the radiosensitizing effects of TAE684 reported here.

NSCLC is one of the most challenging malignancies, although its prognosis has improved due to new therapeutic agents and better combined therapy regimens. The introduction of FDG-PET-CT has reduced the number of falsely classified locally advanced patients and together with improved target volume delineation and radiotherapy techniques contributed to a better patient outcome. Despite all these progresses, long-term survival is still limited in patients presenting at locally advanced or metastatic stages. Thus, personalized therapies based on individual tumor characteristics are urgently needed for NSCLC patients. The development of ALK inhibitors has provided a promising therapeutic opportunity for treatment of advanced metastatic NSCLC [39, 40]. Based on our data, a relatively large fraction of patients with locally advanced disease and ALK-positive tumors may benefit from combined ALK inhibition and radiotherapy. Hence, in addition to the current practice in stage IV disease, routine examination of ALK status might be warranted in locally advanced Stage III NSCLC prior to radiotherapy. In analogy to combined EGFR-inhibition (cetuximab) and radiotherapy in HNSCC, it is conceivable that ALK-inhibition may provide a less toxic alternative to chemotherapy for concurrent treatment of ALK-positive NSCLC with radiotherapy [41]. Our data unequivocally indicate further in-vivo and clinical exploration of this favorable combination in ALK-fusion-harboring NSCLC.

In this report, we demonstrated that concurrent inhibition of ALK in combination with irradiation reduced the proliferative capacity and enhanced apoptosis selectively in human H3122 NSCLC tumors with EML4-ALK translocation. Based on the clonogenic survival data, a synergistic activity was further observed between irradiation and TAE684 treatment in H3122 cells. ALK-inhibition further sensitized NSCLC cells to particle therapy with carbon ions. To our knowledge, this is the first demonstration of potent radiosensitizing effects of TAE684 in NSCLC cells harboring EML4-ALK fusion gene. This study constitutes a critical step towards clinical translation of this favorable combination in NSCLC.