Remarkable response to alectinib for metastatic papillary thyroid cancer with STRN-ALK fusion: A case report

Abstract

Little is known about the efficacy of alectinib for papillary thyroid cancer with STRN-ALK fusion. A 64-year-old female presented with metastatic papillary thyroid cancer, widespread to lungs, mediastinal lymph nodes and brain 20 years after surgery. Disease progression still occurred after radioactive iodine therapy, chemotherapy, and radiotherapy. Tissue obtained from left cervical lymph node confirmed metastatic papillary thyroid cancer. Molecular profiling from re-biopsy tissue identified an STRN-ALK fusion rearrangement. After multidisciplinary discussion, alectinib was administered to the patient. Treatment was well tolerated, and follow-up images confirmed a partial response. ALK occurs rarely, with limited data suggesting the efficacy of ALK inhibitors in thyroid cancer. We presented the first case of a patient with PTC and STRN-ALK fusion to be treat effectively with alectinib.

Introduction

Anaplastic lymphoma kinase (ALK) rearrangement can be detected in various solid tumors, including non-small cell lung cancer, colon cancer, kidney cancer (1). ALK rearrangement is seen in about 5% of all non-small cell lung cancer patients (2). In thyroid cancer, data from TCGA showed the prevalence of ALK rearrangement was 0.8% (3). Currently, little is known about the efficacy of ALK inhibitors on patients with STRN-ALK fusion tumors. Here we present a case showing remarkable response to alectinib for metastatic pulmonary metastases from papillary thyroid cancer with STRN-ALK fusion.

Case presentation

A 64-year-old female was affected by a metastatic papillary thyroid cancer (PTC), widespread to lungs, mediastinal lymph nodes and brain. The treatment timeline is shown in Figure 1. Over the 20 years from the initial diagnosis, the patient underwent total thyroidectomy with central lymph node dissection. The patient also received 2 cycles of radioactive iodine therapy after surgery. After 7 years from surgery, the patient experienced progression of disease (lungs and mediastinal lymph nodes); therefore, another cycle of radioactive iodine therapy was performed. Three years after, the patient experienced progression of disease again (lungs) in 2011. Tissue obtained from lung lesions confirmed metastatic thyroid cancer. Two cycles of pemetrexed (500mg/m2, day 1), carboplatin (AUC=5, day1) and Rh-Endostatin (15mg days 1 to 14) were administrated. The patient showed a partial response of the disease, without grade 3 to 4 adverse events. After 5 years of treatment, progression was confirmed by computed tomography scan (lungs). She also experienced cough and hemoptysis. Imaging showed lung mass near the bronchus, responsible for hemoptysis. Thoracic radiotherapy was carried out with stabilization of the lung metastases and absence of hemoptysis symptoms. Disease remained stable for about 5 years until brain metastasis appeared.

Figure 1

Brain magnetic resonance imaging revealed brain metastasis (right frontal lobe). The patient experienced headache. Fractionate stereotactic radiotherapy (FSRT) was performed with brain metastasis. Headache was relief after FSRT. A computed tomography scan revealed progression of disease in lungs and cervical lymph nodes. Tissue obtained from left cervical lymph node confirmed metastatic papillary thyroid cancer with the immunohistochemistry results of CK (+), TTF-1 (+), CEA (-), and Tg (+). The DNA of re-biopsy tissue was profiled with a capture-based targeted DNA sequencing panel (Burning Rock Biotech, Guangzhou, China) that targets 18 genes (BRAF, NRAS, HRAS, KRAS, RET, NTRK1, ETV6, ALK, PPARG, TERT, EIF1AX, PTEN, AKT1, PIK3CA, TP53, CTNNB1, TSHR, and GNAS) and spans 140 kb of the human genome. STRN-ALK fusion rearrangement (S3:A20) with variant allele fraction (VAF) 33.72% and NRAS (1p13.2) copy number loss were identified by targeted NGS of the biopsy sample.

After multidisciplinary discussion and consent to treatment by the patient, alectinib (600mg twice daily) was administered to the patient. CT and MR scans showed radiological partial response at 1 and 3 months on treatment (Figure 2). The treatment was well tolerated, except for grade 1 diarrhea. To date, the duration of response is more than 8 months. She continues on alectinib.

Figure 2

Discussion

PROFILE 1014 showed ALK inhibitor crizotinib prolonged the survival time compared to chemotherapy in ALK rearrangement NSCLC patients (4). ALEX study showed alectinib had a significantly longer PFS than crizotinib (5). Moreover, the OS benefit of alectinib was seen in patients with brain metastases. STRN-ALK was found as the most common type of ALK fusion (6). Kelly et al. showed ALK inhibitors suppressed thyroid cancer cells harboring STRN-ALK fusion proliferation (6). Currently, there is no randomized control study targeting ALK rearrangement in thyroid cancer. A few researchers found dramatic response of ALK inhibitors in ALK rearrangement thyroid patients. Aydemirli et al. reported a partial response in an EML-ALK fusion patient treated with lorlatinib after resistance to crizotinib (7). de Salins et al. reported a complete response in an ALK rearrangement patient treated with crizotinib (8). In lung cancer, breast cancer and peritoneal mesothelioma, reports had showed the dramatic response of alectinib in patients with STRN-ALK fusion (9–11). While the value of alectinib in patients with STRN-ALK fusion thyroid cancer was unknown.

Currently, more than 90 distinct ALK fusion types have been identified in ALK+ tumors (12). Their response to ALK inhibitors varied differently. Furugaki et al. evaluated the sensitivity to alectinib of eight ALK+ type (EML4-ALK variant 1-4, KIF5B-ALK, KLC1-ALK, STRN-ALK, and TFG-ALK) and no difference were found between them (13).

Conclusion

ALK occurs rarely, with limited data suggesting the efficacy of ALK inhibitors in thyroid cancer. To the best of our knowledge, we presented the first case of a patient with PTC and STRN-ALK fusion to be treat effectively with alectinib.

Funding

This study was supported by grants from Key Project of Hangzhou. The funder had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Acknowledgments

The authors thank the patient for her participation in this study.

Publisher’s note

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