Abstract
Immune checkpoint inhibitors have been recently approved for cancer treatment. Nivolumab is a monoclonal antibody specific for programmed cell death-1 (PD-1) that modulates T-cell response. It was initially used for the treatment of malignant melanoma and then approved in other cancers, such as non-small cell lung cancer and clear cell renal cell carcinoma (ccRCC). So far, the activity of nivolumab in patients with thyroid malignancies has been reported in a single case of anaplastic thyroid cancer. Here, we report the case of a patient with ccRCC who developed a papillary thyroid carcinoma (PTC) under first-line sunitinib treatment. During nivolumab, the second-line treatment for ccRCC, we unexpectedly observed a complete regression of PTC.
Established Facts
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It is already known that papillary thyroid cancer arising in a background of Hashimoto thyroiditis shows increased programmed cell death-1 (PD-L1).
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It is already known that metastases to the thyroid gland are uncommon, but frequently associated with renal cancer, especially when presenting as a fast growing nodule.
Novel Insights
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Our case strongly supports the evaluation of nivolumab and possibly other forms of immune therapy in the treatment of papillary thyroid carcinoma.
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The presence of histiocyte aggregates on the site where the prior nodule had been observed supports the hypothesis of an immune-mediated tumor regression.
Introduction
Immune checkpoint inhibitors have been recently approved for cancer treatment. Programmed cell death-1 (PD-1) and cytotoxic T-lymphocyte antigen 4 (CTLA-4) are checkpoint proteins expressed on the surface of cytotoxic T-cells which interact with their ligands to regulate immune response in physiologic conditions. Monoclonal antibodies that target either PD-1 or its ligands (e.g., PD-L1) can restore the host immune reaction against cancer cells [1]. Nivolumab is a monoclonal antibody specific for PD-1 that modulates T-cell response. It was initially used for the treatment of malignant melanoma and then approved in other cancers, such as non-small cell lung cancer and clear cell renal cell carcinoma (ccRCC) [2]. More recently, a case of anaplastic thyroid cancer treated with vemurafenib and nivolumab has been described, achieving substantial regression and complete radiographic and clinical remission [3].
Case Report
In February 2014, a 54-year-old male was referred to our center, 1 month after resection of a right ccRCC pT1a, with evidence of two suspect osteolytic lesions localized in the L1 and L2 vertebrae. A bone biopsy was performed, confirming the presence of carcinoma cells compatible with ccRCC. The prognostic Motzer risk score, which is used to predict patient prognosis based on clinical and hematological parameters [4], was intermediate (i.e., around 10–12 months). In March, the patient received antalgic radiation therapy to L1 and L2 for a total dose of 36 Gy and was then started on first-line sunitinib 50 mg per day (4-weeks-on/2-weeks-off schedule) and zoledronic acid. In April 2014, due to G2 asthenia and G2 hand-foot syndrome, the sunitinib schedule was switched to 2-weeks-on/1-week-off, with better tolerability. In February 2015, due to worsening of hand-foot syndrome, the dose of sunitinib was reduced to 37.5 mg per day (Fig. 1), which the patient continued until November 2017 due to stability of the bone lesions at periodic CT and MRI scans.
As often observed during treatment with sunitinib [5], in November 2014 the patient presented subclinical hypothyroidism (Fig. 1), with negative antibodies against thyroglobulin and thyroperoxidase. No L-thyroxine replacement therapy was initiated. The neck ultrasound (US) showed a thyroid gland of normal volume, without nodules or parenchymal abnormalities. Serological values of TSH normalized without therapy in March 2015, after reduction of the sunitinib dose. In July 2016, the follow-up neck US showed a thyroid micronodule (4 × 4 × 5 mm, vol 0.042 mL) solid in nature, strongly hypoechoic, with taller-than-wide shape, ill-defined margins, and little peripheral vascularity on Doppler US. Based on the small dimensions of the nodule, periodic US follow-up was scheduled.
In October 2017, spine MRI scans showed appearance of a suspect metastatic bone lesion in C4 vertebra. Bone scintigraphy, performed in November 2017, confirmed tracer hyper-fixation in the cervical spine. The patient refused radiation therapy, and second-line therapy with nivolumab was planned for December 2017.
Before starting nivolumab, the patient underwent follow-up neck US, in which a significant volumetric increase in the nodule was detected (dimensions of 14 × 10 × 18 mm, vol 1.3 mL) (Fig. 2a), and fine needle aspiration was performed. Cytological smears showed scanty atypical thyrocytes in a bloody background. These cells had overlapping oval nuclei with grooves (Fig. 2b) and were positive for thyroid transcription factor 1 (TTF1) immunostaining (Fig. 2c). The diagnosis was of cytology suspicious for papillary thyroid carcinoma (PTC), category TIR4 according to the Italian consensus for the classification and reporting of thyroid cytology [6]. Based on the cytology and the radiological evolution of the lesion, a diagnosis of PTC was made. After a multidisciplinary meeting, in consideration of the progressive bone disease secondary to ccRCC, it was decided to postpone thyroidectomy and to start treatment with nivolumab as planned.
Nivolumab was started in December 2017, with good tolerability. In March 2017, a minimally progressive disease was recorded (appearance of small non-painful bone lesions in D9, D11, and D12 vertebrae), but treatment was continued beyond progression in absence of cancer-related symptoms. At the last available scans (November 2018), the bone lesions were stable in dimension. Treatment with nivolumab is still ongoing.
At the 6-month follow-up visit after detection of PTC (i.e., in July 2017 after 6 months of nivolumab therapy), the neck US showed a thyroid gland with slightly irregular texture, without clear evidence of the previously diagnosed nodule. In order to confirm the regression of the lesion, a thyroid core biopsy was performed on the site where the prior nodule had been observed. Microscopic evaluation of the core showed a thyroid parenchyma with normal follicles and lymphomonocytic infiltrate, as observed in thyroiditis (Fig. 3a). An area of focal cellular reaction with histiocyte aggregates was observed and confirmed by immunohistochemistry for CD68 (Fig. 3b). Immunostaining for CD4 and CD8 showed CD4-positive lymphocytes and histiocytes (Fig. 3c), without relevant presence of CD8-positive lymphocytes. The final diagnosis was chronic thyroiditis with focal granulomatous features and no residual cancer. Follow-up neck US, as well as TSH and FT4 values have been stable within normal limits so far.
Discussion
The association between a first diagnosis of ccRCC and a subsequent thyroid cancer is strong and often underrecognized by clinicians. Although, as in our case, it might be partially explained as a result of continued surveillance bias [7]. Metastases to the thyroid gland are uncommon, but frequently associated with renal cancer, especially when presenting as a fast growing nodule as in our case [8]. For this reason, we performed TTF1 immunostaining on the cytological sample, which confirmed the thyroidal origin.
PTC accounts for approximately 85% of thyroid cancers and is generally associated with a good prognosis. Treatment modalities most often include surgery and radioiodine therapy. Systemic therapies with tyrosine kinase inhibitors are reserved for metastatic radioiodine-resistant cases [9]. Interestingly, in our patient, PTC was originally diagnosed when the patient was under treatment with the tyrosine kinase inhibitor sunitinib, possibly an even rarer occurrence. In animal models, TSH stimulation contributes to the development of thyroid cancer, and high serum TSH has been associated with higher risk of thyroid cancer in patients with thyroid nodules [10]. It is difficult to establish whether fluctuating levels of TSH over time might have influenced the development and growth of PTC in our case.
Since tyrosine kinase inhibitors as well as immune checkpoints inhibitors may induce thyroid dysfunction and thyroiditis [11, 12], cytopathologists should carefully consider the interpretation of nuclear changes, such as clearing or membrane irregularities, mimicking papillary carcinoma. In thyroiditis, however, nuclear alterations are usually mild and focal. In our case, well-developed papillary nuclear features were observed in bloody, paucicellular smears. Due to this limiting factor, the pathological report was classified as suspicious for papillary carcinoma.
The therapeutic effect of nivolumab monotherapy in ccRCC has been reported in phase III clinical trials. In this study, nivolumab showed a significantly longer overall survival compared to the mTOR inhibitor everolimus [13]. On the contrary, the use of checkpoint inhibitors is not part of the standard therapeutic algorithm for PTC [14]. Positivity of PD-L1 has been in fact consistently reported in PTC, especially in aggressive cases [15-20], as well as in a subset of patients with advanced follicular and anaplastic thyroid cancers [21]. In particular, PTC arising in a background of Hashimoto thyroiditis shows increased PD-L1 expression [22]. Whether the sunitinib-induced thyroid dysfunction might be associated with increased PD-L1 expression is only speculative. Although our patient was eventually diagnosed with a chronic thyroiditis, autoantibodies were negative during the diagnostic workup. The presence of histiocyte aggregates supports the hypothesis of an immune-mediated tumor regression. Other potential biomarkers predictive of response to checkpoint inhibitors have also been assessed in PTC: the tumor mutation burden is generally low – consistent with what is observed with other endocrine tumors – although immunogenic mutation might still be present [23]. Finally, the presence of a lymphocytic infiltrate in PTC has shown controversial prognostic associations, with most reports, however, suggesting an anti-tumoral role of the inflammatory milieu [24, 25].
From a clinical perspective, the case of a patient with anaplastic thyroid carcinoma responding to nivolumab treatment was recently reported [3]. Ongoing trials are still formally evaluating the potential role of immunotherapy in advanced thyroid cancers; specifically, nivolumab is being tested in a phase II trial alone or in combination with ipilimumab (a CTLA-4 inhibitor) in metastatic, radioiodine-refractory, differentiated thyroid cancers (NCT03246958). Our case strongly supports the evaluation of nivolumab and possibly other forms of immune therapy in the treatment of PTC.
Statement of Ethics
Ethics approval and consent to participate: not applicable. Consent for publication: an institutional consent form for data publication was obtained from the patient.
Disclosure Statement
The authors have no conflicts of interest to declare.
Funding Sources
No funding was received for the writing of this paper.
Author Contributions
A.P. and A.N.: patient management, figure preparation, manuscript writing. D.M. and S.M.: patient management. A.M.N. and G.T.: patient management, manuscript writing. A.C. and C.T.: pathological analysis. F.P.: patient management, manuscript writing.G.T.: patient management, manuscript editing. D.S.: patient management, manuscript writing, manuscript editing.
Footnotes
verified
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