Internal Medicine Resident Physician Atlantic Health Summit, NJ, United States
Background: SDHA-related paragangliomas (PGLs) have been historically considered low penetrance with limited metastatic risk. Emerging evidence suggests a more aggressive phenotype, with reports of delayed metastases occurring 16–37 years after diagnosis. Case series indicate that up to 5 of 32 SDHA-mutated PGLs develop metastases, supporting an intermediate-to-high risk profile. We present a case of metastatic SDHA-PGL (c.771-1G>C variant) at initial presentation.
Clinical
Case: A 34-year-old man with no history of hypertension, catecholamine-related symptoms, or known family history presented with left-sided neck pain and a progressively enlarging mass over one year. Initial MRI revealed a 3.9 × 3.6 × 4.5 cm left carotid space mass; surgical intervention was delayed by the patient. Plasma metanephrine and normetanephrine levels were within normal limits (41 pg/mL [ref < 57] and 97 pg/mL [ref < 148], respectively). Functional imaging demonstrated Stage IV disease with DOTATATE-avid cervical mass and metastatic involvement of the cervical, thoracic, and lumbar spine, iliac wing, and liver. More than one year after presentation, the patient underwent uncomplicated resection of a 4 cm PGL. Pathology demonstrated loss of SDHB expression with retained fumarate hydratase, chromogranin and synaptophysin positivity, and S100-positive sustentacular cells. Seven lymph nodes were negative, with no lymphovascular or perineural invasion. No locoregional recurrence was identified at 3-month follow-up. Given high-volume metastatic disease, oncology recommended treatment with 177Lu-DOTATATE (Lutathera) in combination with somatostatin analogues following multidisciplinary discussion. Treatment initiation has been deferred due to fertility preservation considerations. Germline testing revealed a likely pathogenic SDHA splice-acceptor variant (c.771-1G>C), associated with autosomal dominant hereditary PGL-pheochromocytoma syndromes and overlapping mitochondrial complex II deficiency disorders. SDHA variants have also been linked to gastrointestinal stromal tumors, renal cell carcinoma, and pituitary adenomas.
Conclusion: SDHA-PGL should not be considered a low-risk entity. Literature demonstrates metastatic rates similar to SDHB in some cohorts, contradicting earlier assumptions of low risk. Even in the absence of catecholamine excess, SDHA-PGL warrant lifelong biochemical and imaging surveillance and genotype-informed counseling. SDHA-mutated tumors may grow slowly yet metastasize decades after initial resection, emphasizing the need for lifelong follow-up. MRI, low dose Chest CT, and DOTATATE PET are the preferred surveillance modalities. The presented c.771-1G>C variant expands the known pathogenic and clinical spectrum of SDHA PGLs. This specific genotype has very limited published characterization.
PMID: 39133175
*Unless otherwise noted, all abstracts presented at ENDO must not be released to the press or the public until the date and time of presentation. For oral presentations, the abstracts are embargoed until the session begins. The Endocrine Society reserves the right to lift the embargo on specific abstracts that are selected for promotion prior to or during ENDO.*
.jpg)
.jpg)