Synchronous Adrenocortical Carcinoma, Renal Cell Carcinoma, and Mediastinal Mature Teratoma with Heterozygous Variants in SMARCA4, APC, and MYBP3: A Case Report

Ferit ASLAN; Burcu ERKILIÇ; Şeref Barbaros ARIK; Fisun ARDIÇ YÜKRÜK; Ersin ATABEY; Fatih YILDIZ; Hakan TABAN

doi:10.37047/jos.galenos.2026.2025-10-7

ABSTRACT

We describe an exceptionally rare case of a 46-year-old woman diagnosed with three synchronous primary tumors: adrenocortical carcinoma (ACC), renal cell carcinoma (RCC), and an anterior mediastinal mature teratoma. Cross-sectional imaging demonstrated distinct lesions of comparable size (each measuring 6-7 cm) in the right adrenal gland, right kidney, and the mediastinum. The patient underwent radical nephrectomy, adrenalectomy, and excision of the mediastinal mass. Histopathology confirmed clear cell RCC, ACC, and a mature teratoma without malignant transformation. Molecular testing revealed heterozygous variants in SMARCA4, APC, and MYBP3, suggesting a permissive background for multiple tumorigenic events. Importantly, all tumors were diagnosed at an early stage and completely resected, thereby enabling curative surgery without the need for adjuvant therapy. This unique presentation underlines the importance of integrated radiological, pathological, and molecular evaluation in patients with multiple synchronous tumors and highlights the role of vigilant follow-up in long-term management.

Keywords:

Adrenocortical carcinoma, renal cell carcinoma, mediastinal mature teratoma, SMARCA4 variant, synchronous primary tumors

INTRODUCTION

The occurrence of multiple synchronous primary tumors is uncommon and often poses diagnostic as well as therapeutic challenges. While some cases are associated with well-defined hereditary cancer syndromes such as Li-Fraumeni, Lynch, or von Hippel-Lindau disease, the coexistence of independent tumors outside these classical syndromes is exceedingly rare.^1-3

Adrenocortical carcinoma (ACC) and renal cell carcinoma (RCC) have occasionally been reported in combination, and mediastinal germ cell tumors are recognized entities, but the simultaneous presence of ACC, RCC, and a mediastinal mature teratoma of comparable size in the same patient has not previously been described.^4-6 Rare reports have described atypical RCC presentations with poor prognosis.⁷ In contrast, our patient presented with three synchronous tumors that were completely resected at an early stage, allowing curative surgery without the need for adjuvant therapy.

Molecular profiling revealed heterozygous variants in SMARCA4, APC, and MYBP3, suggesting a permissive genetic background for multiple tumorigenic events. This emphasizes the importance of integrating radiological, pathological, and molecular evaluation in patients with rare tumor associations, where clinical outcomes may vary widely depending on stage and genetic profile.

CASE REPORT

A 46-year-old woman presented with a two-week history of retrosternal chest pain. The physical examination was unremarkable. Thoracic computed tomography (CT) revealed a 6.2 cm anterior mediastinal mass with cystic and necrotic components, while abdominal CT demonstrated two distinct lesions: a 6.5 cm heterogeneously enhancing mass in the upper pole of the right kidney and a 6.7×5.1 cm well-circumscribed adrenal mass (Figure 1).

Fluorodeoxyglucose positron emission tomography/CT confirmed metabolic activity in all three lesions (maximum standardized uptake value: mediastinal 2.19, renal 3.32, adrenal 11.58) without evidence of distant metastasis. A comprehensive endocrine evaluation, including measurements of cortisol, dehydroepiandrosterone sulfate, aldosterone, and catecholamines, as well as an overnight dexamethasone suppression test, revealed no hormonal excess, a finding consistent with a non-functioning ACC. Additionally, tumor markers commonly associated with germ cell tumors—alpha-fetoprotein, beta human chorionic gonadotropin, and lactate dehydrogenase—were within normal limits, supporting the diagnosis of a benign mediastinal teratoma.

The patient underwent right radical nephrectomy, right adrenalectomy, and excision of the mediastinal mass. Histopathological analysis confirmed three independent primary tumors (Figure 2).

• Renal tumor: Clear cell RCC, World Health Organization/International Society of Urological Pathology grade 2, confined to kidney, paired box gene 8 and epithelial membrane antigen positive.

• Adrenal tumor: ACC, Weiss score 3, inhibin and Melan-A positive, non-functioning.

• Mediastinal mass: Mature teratoma composed of gastrointestinal, pancreatic, thymic, and mesenchymal elements, without malignant transformation.

Molecular analysis identified heterozygous variants in SMARCA4, APC, and MYBP3, while no alterations were detected in classical hereditary cancer genes. Importantly, both RCC and ACC were diagnosed at an early stage and were completely resected; therefore, no adjuvant systemic therapy was indicated. The patient has been followed for 20 months after surgery without evidence of recurrence.

DISCUSSION

The coexistence of three distinct primary tumors in a single patient is exceptionally rare and raises multiple clinical, prognostic, and molecular questions. In the setting of synchronous tumors, outcomes are often worse than for solitary primaries, largely due to diagnostic complexity, increased cumulative tumor burden, or limited therapeutic options. In one large series, the 1-year survival was 56.9%, but the 3-year survival dropped to 20.9%.⁸ Other population-based data confirm that synchronous metastases are associated with a poorer prognosis than metachronous ones.^{9, 10} Case reports also emphasize the rarity and clinical challenges of managing synchronous malignancies.¹¹

Demographically, most published reports of synchronous tumors involve middle-aged or older patients, often with a slight male predominance. Younger age has occasionally been associated with better outcomes, whereas unusual presentations in women have also been described in the literatüre.^{7, 8} These observations underline the importance of age and sex as potential prognostic modifiers in synchronous malignancies.

Clinically, both RCC and ACC were diagnosed at an early stage in our patient. Radical nephrectomy and adrenalectomy achieved complete resection; given the absence of adverse pathological features or hormonal activity, adjuvant systemic therapy was not required. The mediastinal teratoma was also completely excised and confirmed as benign. At 20 months’ follow-up, the patient remains recurrence-free, demonstrating that early detection and curative surgery can mitigate the otherwise poor prognosis often reported for synchronous tumors.

From a molecular perspective, heterozygous variants in SMARCA4, APC, and MYBP3 were identified. SMARCA4 is a catalytic subunit of the switch/sucrose non-fermentable chromatin-remodeling complex, and its inactivation has been strongly linked to aggressive tumor biology. In small cell carcinoma of the ovary and thoracic sarcomas, SMARCA4-deficient tumors are associated with poor prognoses; median survival is often below one year.^{1, 2} In non-small cell lung cancer, SMARCA4 alterations similarly predict shorter overall and progression-free survival.^{3, 12} Interestingly, some studies suggest that SMARCA4-deficient tumors may respond more favorably to immune checkpoint inhibitors, raising the possibility of immunotherapy as a targeted therapeutic strategy.^12-14

APC mutations, by contrast, are central to Wnt/β-catenin pathway activation and have been associated with colorectal and adrenal carcinogenesis, often contributing to aggressive tumor biology.^{4, 5} MYBP3 variants, although less well characterized, have been reported in pan-cancer sequencing efforts and may reflect underlying genomic instability rather than acting as true driver mutations.⁶

In our patient, the coexistence of three synchronous tumors harboring molecular alterations contrasts with the otherwise favorable clinical outcome achieved following complete resection. This underscores the importance of multidisciplinary evaluation: while genetic findings raise concerns for long-term risk, the absence of recurrence after nearly two years highlights that surgical management at an early stage remains the most decisive prognostic factor. Future studies may clarify whether patients with SMARCA4-altered tumors should benefit from closer surveillance or early inclusion in immunotherapy protocols.

CONCLUSION

This case represents an exceptionally rare coexistence of three synchronous primary tumors: RCC, ACC, and a mediastinal mature teratoma. Despite harboring molecular alterations including heterozygous SMARCA4, APC, and MYBP3 variants—changes usually associated with aggressive behavior—the patient achieved a favorable outcome with curative surgery alone. At 20 months’ follow-up, she remains disease-free without adjuvant systemic therapy. This case highlights that early-stage diagnosis and complete resection can outweigh adverse molecular markers while emphasizing the importance of vigilant follow-up and the consideration of molecular risk in surveillance planning.

Ethics

Informed Consent: Informed consent was obtained from the patient and the patient’s family for publication of the case report.

Authorship Contributions

Surgical and Medical Practices: F.A., Ş.B.A., F.A.Y., E.A., F.Y., H.T., Concept: F.A., B.E., H.T., Design: F.A., B.E., H.T., Data Collection or Processing: F.A., B.E., Ş.B.A., F.A.Y., E.A., H.T., Analysis or Interpretation: F.A., Ş.B.A., F.A.Y., E.A., F.Y., Literature Search: F.A., B.E., Writing: F.A., B.E.

Conflict of Interest: No conflict of interest was declared by the authors.

Financial Disclosure: The authors declared that this study received no financial support.

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