05 February 2026: Articles 
Giant Cell Arteritis/Polymyalgia Rheumatica and Atypical Pulmonary Carcinoid Tumor: A Paraneoplastic Syndrome?
Rare coexistence of disease or pathology
Omar Al Tabaa
ABE 1*, Sabrina Hamroun E 1, Khaled Al Tabaa F 2, Roxana Poll A 3, Waad Al Sheikh A 4, Edouard Pertuiset AEF 1
DOI: 10.12659/AJCR.950346
Am J Case Rep 2026; 27:e950346
Abstract
BACKGROUND: Giant cell arteritis (GCA) is the most common large-vessel vasculitis in individuals over age 50 years. Although it typically affects extracranial branches of the carotid artery, central nervous system involvement is rare and can manifest with ischemic stroke. Links between GCA and malignancy have been reported, especially hematologic cancers, but paraneoplastic GCA associated with solid tumors remains exceptional and poorly understood.
CASE REPORT: We describe a 59-year-old man presenting with temporal headaches, right-hand paresthesia, monocular visual loss, and gait instability. Imaging revealed left thalamic ischemia and bilateral vertebral artery stenosis without atherosclerosis. Examination and Doppler ultrasound supported a diagnosis of GCA with associated polymyalgia rheumatica (PMR), although a temporal artery biopsy was negative. Inflammatory markers were only moderately elevated, consistent with reports of GCA cases with ischemic complications. PET-CT incidentally identified a mediastinal mass, confirmed as small-cell pulmonary neuroendocrine carcinoma. Symptoms improved with corticosteroids, but tapering below 15 mg/day caused relapse, requiring methotrexate. Despite partial oncologic response, brain metastases appeared 8 months later. Follow-up vascular imaging showed regression of arterial stenoses under corticosteroids, arguing against atherosclerosis and supporting the inflammatory nature of the lesions. GCA manifestations remained corticosteroid-dependent throughout follow-up.
CONCLUSIONS: The simultaneity of GCA and lung neuroendocrine carcinoma, persistence of corticosteroid dependence, and lack of remission despite oncologic response strongly suggest a paraneoplastic mechanism. This case emphasizes the need for heightened suspicion of underlying cancer in patients with atypical, biopsy-negative, or treatment-resistant vasculitis. Recognition of paraneoplastic GCA may improve early cancer detection and influence management decisions at the intersection of rheumatology and oncology.
Keywords: Paraneoplastic Syndromes, Polymyalgia Rheumatica, Vasculitis
Introduction
Giant cell arteritis (GCA) is the most common type of large- and medium-vessel vasculitis in individuals over 50 years of age. While GCA typically affects the extracranial branches of the carotid artery, it can rarely involve the central nervous system, leading to ischemic strokes with significant prognostic implications [1].
Paraneoplastic syndromes, which are systemic manifestations of malignancy triggered by immune or humoral factors (rather than tumor invasion), are extremely rare in vasculitides [2]].
Paraneoplastic vasculitis, a subtype, is typically associated with hematologic cancers [3], and only a small number of cases have linked GCA with malignancies [4,5]. Therefore, given the rarity of this entity, it is necessary to document cases to better understand its pathophysiology.
We report a rare case of ischemic stroke revealing GCA, diagnosed concurrently with pulmonary neuroendocrine carcinoma, suggesting a paraneoplastic syndrome.
Case Report
A 59-year-old man, who was a current smoker with a history of chronic obstructive pulmonary disease and sleep apnea, was admitted in June 2024 for neurological symptoms. He had been experiencing temporal headaches for 3 weeks and balance disturbances for 2 weeks, along with right-hand paresthesia and a transient monocular vision loss episode in the left eye.
Brain MRI revealed a left thalamic ischemic stroke with FLAIR hypersignal in the right temporal artery, with no associated suspicious lesions. CT angiography showed significant stenosis of both vertebral arteries and the left carotid siphon, without evidence of atherosclerosis. He had no cardiovascular risk factors other than smoking.
Examination revealed temporal artery induration and hyperesthesia of the scalp. The patient also had shoulder and hip girdle pain consistent with polymyalgia rheumatica (PMR). C-reactive protein (CRP) was 15 mg/L and erythrocyte sedimentation rate (ESR) was 35 mm/h. Temporal artery Doppler imaging showed a right frontal branch halo sign (Figure 1), while a temporal artery biopsy (TAB) was negative. There was no evidence of an infectious cause, and blood cultures were negative, ruling out endocarditis.
Positron-emission tomography–computed tomography (PET-CT) revealed no vascular hypermetabolism but showed findings suggestive of PMR and a large hypermetabolic mediastinal mass (Figure 2A). Biopsy identified a small-cell neuroendocrine carcinoma of the lung.
The patient received 3 intravenous pulses of 500 mg methylprednisolone, followed by 1 mg/kg/day prednisone. All his symptoms resolved rapidly, and inflammatory markers normalized. Chemotherapy with carboplatin and etoposide was initiated.
In October 2024, a follow-up PET-CT scan showed partial oncologic response and resolution of PMR signs (Figure 2B). Corticosteroid tapering was limited by recurrence of symptoms at below 15 mg/day (increase in headaches, hyperesthesia of the scalp and biological inflammatory markers), prompting the addition of 15 mg methotrexate per week, orally, which failed to reduce corticosteroid requirements after 3 months.
A follow-up cerebral MRI was performed in early December 2024, showing improvement in cranial arterial stenoses with no recurrence of ischemia and no sign of malignancy. There was regression of the hypersignal in the right temporal artery, which retained normal caliber and enhancement, as well as regression of bilateral carotid stenosis.
In February 2025, the patient developed peripheral facial palsy. Brain imaging revealed both supra- and infra-tentorial metastases, along with a right adrenal lesion, indicating cancer progression. Chemotherapy was resumed, along with brain radiotherapy.
As of the latest follow-up, the patient remains corticosteroid-dependent at 20 mg/day, with no active signs of GCA, and is continuing oncological management.
Discussion
This case involved a rare and complex presentation of GCA diagnosed concurrently with a solid tumor; specifically, a small-cell neuroendocrine carcinoma of the lung. The significant hypermetabolism on PET-CT (SUV max 10.9) suggested an atypical carcinoid tumor. The simultaneity of both conditions raises the possibility of a paraneoplastic mechanism. While the literature has explored the association between GCA and malignancies, particularly hematologic ones, links with solid tumors remain uncommon and poorly understood [4,5].
From a diagnostic standpoint, the patient fulfilled the ACR/EULAR 2022 classification criteria for GCA [6], including characteristic clinical symptoms, Doppler findings (halo sign), and PMR features. However, certain atypical aspects of the presentation warranted a thorough differential diagnosis. The negative temporal artery biopsy (TAB), although not uncommon given its limited sensitivity [7], and a relatively low CRP level (15 mg/L), raised the question of alternative diagnoses. However, studies have shown that GCA cases presenting with ischemic complications often exhibit lower CRP levels, possibly due to localized vascular inflammation rather than systemic inflammation [8–11].
Several differential diagnoses needed to be considered. Atherosclerosis was initially contemplated, given the vascular stenoses observed on imaging. However, the absence of significant cardiovascular risk factors – apart from smoking – and the lack of atherosclerotic calcifications or plaques on CT angiography made this diagnosis unlikely. More importantly, the improvement of the vascular stenoses on follow-up imaging after corticosteroid therapy argued strongly against atherosclerosis, which would not be expected to show such reversibility.
An infectious etiology, particularly endocarditis, was also ruled out. Other forms of systemic vasculitis, such as ANCA-associated vasculitis, were excluded based on the absence of renal involvement, pulmonary hemorrhage, or positive autoantibodies. Similarly, primary central nervous system vasculitis seemed improbable, given the presence of extracranial features (scalp hyperesthesia, and temporal artery abnormalities) and symptoms suggestive of polymyalgia rheumatica.
Taken together, these elements supported the diagnosis of GCA despite some atypical findings.
While the concurrent diagnosis of cancer and GCA could be coincidental, there appears to be no increased risk of malignancy after a GCA diagnosis [12]]. The patient’s smoking habit was a major risk factor for the malignancy.
The simultaneous occurrence of GCA and neuroendocrine carcinoma, along with persistent corticosteroid dependency prior to tumor progression, supports a potential paraneoplastic mechanism. Indeed, temporal relationship between tumor diagnosis and rheumatic symptoms is the main critical issue [2]. A syndrome is generally considered either paraneoplastic, when its musculoskeletal manifestations appear simultaneously or within 1 year and in some studies up to 2 years before the detection of the malignancy. Another important argument is that total elimination of the tumor induces complete remission of paraneoplastic symptoms. This could not be achieved in our patient, who did not benefit from optimal treatment due to his underlying pulmonary pathology.
While few associations between GCA and malignancies, particularly hematological cancers, have been documented, paraneoplastic GCA remains exceedingly rare [4,5].
Deshayes et al reported 49 GCA patients with concurrent malignancy. There were more cases of PMR in the GCA with concurrent malignancy group than in the comparative group (55% vs 34% respectively,
Regarding pathophysiology, the mechanisms underlying paraneoplastic vasculitis, including GCA, are not fully elucidated. The immunological hypothesis is plausible: tumors may secrete antigens or induce immune responses that trigger vasculitis via cross-reactivity. Notably, large-vessel vasculitis, including GCA, has been reported as a complication of immune checkpoint inhibitors, reinforcing the idea of T-cell-mediated vascular injury in response to tumor antigens [13]. The neuroendocrine tumor could potentially share antigenic similarities with vascular structures, or secrete pro-inflammatory cytokines, favoring vasculitic phenomena.
Conclusions
This case highlights an exceptionally rare association between giant cell arteritis and a solid tumor, specifically a small-cell neuroendocrine carcinoma of the lung. While GCA has been sporadically reported in association with hematologic malignancies, its occurrence as a paraneoplastic manifestation of solid tumors remains extremely uncommon and poorly characterized. The simultaneous onset of symptoms, along with persistent corticosteroid dependency prior to tumor progression, supports a potential paraneoplastic mechanism, likely of immunological origin. This is in line with emerging evidence linking large-vessel vasculitis to immune dysregulation in oncologic contexts, such as with immune checkpoint inhibitors [13].
Clinically, this case underscores the importance of considering underlying malignancy in patients with atypical features of GCA, particularly when there is low systemic inflammation, negative biopsy, or persistent corticosteroid dependence.
Future studies could help clarify whether certain neoplasms are more likely to trigger vascular inflammation, and how this might influence diagnostic and therapeutic strategies.
Figures
Figure 1. Halo sign of the right frontal branch temporal artery on Doppler ultrasound. 
Figure 2. PET-TDM. (A) PET-TDM at diagnosis on June 2024 showing large, intensely hypermetabolic mediastinal lesion (white arrow) and bilateral scapulohumeral hypermetabolic involvement of moderate intensity associated with metabolic involvement in favor of cervical and lumbar bursitis and bilateral trochanteric involvement (black arrows), with no significant vascular metabolic damage to medium-large-caliber arteries. (B) PET-TDM on October 2024 showing disappearance of periarticular metabolic activity in the limb girdles and decrease in hypermetabolic mass of posterior mediastinum. SUV max 8.9 and VTM 15.9 cm2 versus SUV max 10.9 and VTM 59.3 cm2. References
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2. Manger B, Schett G, Rheumatic paraneoplastic syndromes – A clinical link between malignancy and autoimmunity: Clin Immunol, 2018; 186; 67-70
3. Solans-Laqué R, Bosch-Gil JA, Pérez-Bocanegra C, Paraneoplastic vasculitis in patients with solid tumors: Report of 15 cases: J Rheumatol, 2008; 35(2); 294-304
4. Deshayes S, Liozon E, Chanson N, Concomitant association of giant cell arteritis and malignancy: A multicenter retrospective case-control study: Clin Rheumatol, 2019; 38(5); 1243-49
5. Liozon E, Loustaud V, Fauchais AL, Concurrent temporal (giant cell) arteritis and malignancy: Report of 20 patients with review of the literature: J Rheumatol, 2006; 33(8); 1606-14
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7. Rubenstein E, Maldini C, Gonzalez-Chiappe S, Sensitivity of temporal artery biopsy in the diagnosis of giant cell arteritis: A systematic literature review and meta-analysis: Rheumatology, 2020; 59(5); 1011-20
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13. Cottu A, Delaval L, Forestier A, Immune checkpoint inhibitors-induced large vessel vasculitis: Clinical characteristics and management from a European multicentre study: Rheumatol (Oxford), 2025; 64(8); 4564-54
Figures
Figure 1. Halo sign of the right frontal branch temporal artery on Doppler ultrasound.Figure 2. PET-TDM. (A) PET-TDM at diagnosis on June 2024 showing large, intensely hypermetabolic mediastinal lesion (white arrow) and bilateral scapulohumeral hypermetabolic involvement of moderate intensity associated with metabolic involvement in favor of cervical and lumbar bursitis and bilateral trochanteric involvement (black arrows), with no significant vascular metabolic damage to medium-large-caliber arteries. (B) PET-TDM on October 2024 showing disappearance of periarticular metabolic activity in the limb girdles and decrease in hypermetabolic mass of posterior mediastinum. SUV max 8.9 and VTM 15.9 cm2 versus SUV max 10.9 and VTM 59.3 cm2. In Press
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