Glomus jugulare tumours (GJT) are benign tumours that grow from the chemoreceptor tissue of the jugular bulb. They are characterised by locally destructive growth into adjacent bones and tissues and frequent recurrence. Their estimated annual incidence has been reported about 0.07 case per 100,000 per year.¹ Surgery with or without preoperative transarterial embolisation may be used in the treatment of GJT, but it has significant morbidity and mortality.² An alternative to surgery is normofractionated external radiotherapy, through which high level of local control can be achieved.³ However, due to the high probability of long-term patient survival after treatment, patients are very likely to experience serious late toxicity, particularly ototoxicity, neurotoxicity, cognitive dysfunction or dysphagia and possible induction of secondary tumours.⁴ Another option is stereotactic radiotherapy (SRT), which can achieve improved dose distribution. However, in general, SRT is only suitable for small target volumes and delivers low-dose radiation to a large volume of healthy tissue.⁵ This limitation could be overcome using proton beam, which offer zero exit dose and lower dose in front of the target volume (Bragg peak). Proton therapy may be technique of choice in reducing the dose to critical organs, especially in larger target volumes and the most in laterally located tumours. The aim of this retrospective study is to evaluate the feasibility, dosimetry, acute and late toxicity and therapeutic response in patients treated with pencil-beam scanning proton radiotherapy. Twelve evaluated patients is the largest study of proton therapy for GTJ.

Between December 2013 and August 2020, 12 patients with GJT were treated with IMPT and they were evaluated in this retrospective study. Nine patients had unilateral tumours, two had bilateral tumours, and one had a unilateral tumour with liver and lung metastatic involvement at the time of radiation treatment. The median dose was 54 GyE (Gray Equivalents) (50–60 GyE) with daily fractions of 2 GyE. The standards constraints for head and neck region were used, and they were corrected to higher proton radiobiological efficiency by multiplying factor 1.1.⁶ These constraints were almost always reached, except the closely spreaded tumours in the case of cochlea and inner ear.

Twelve patients were analysed with a median follow-up time of 42.2 months (11.3–86.7). Median of age was 46.5 years. Ten patients were female, and two patients were male. Eight patients underwent primary proton therapy (due to inoperability), two had previous surgery, two had transarterial embolisation before radiotherapy, and one had photon radiotherapy in the past. Demographic and treatment parameters are shown in Table 1.

Table 1 Patient demographic and treatment parameters.

Patients were irradiated in supine position using standard 5-point thermoplastic masks (Orfit Industries, Wijnegem, Belgium). The planning CT was performed with 1.25 mm slice thickness. Dental fillings and metal teeth bridges were removed prior to planning CT in order to reduce CT artefacts. Gadolinium contrast-enhanced MRI was performed in all cases, and images were fused with the planning CT for target volume delineation purposes.

The contouring of target volumes and at-risk organs was performed using Focal software (Elekta AB, Stockholm, Sweden). The gross tumour volume (GTV) included tumour mass visible on MRI, see Figure 1. The clinical target volume (CTV) was not defined. The planning target volume (PTV) was created by expansion of the GTV by 3–5 mm at the discretion of the attending physician based on uncertainty in CT and MRI image fusion and treatment set-up uncertainty. The following critical organs were contoured and included in treatment plan optimisation: the spinal cord, brain stem, inner ear, brain, pharyngeal constrictors, larynx and parotid glands.

Enlarge this image.

Figure 1. MRI typical tumour location.

The prescribed dose for PTV was 50–60 GyE in 25–30 fractions depending on the extent of the tumour and the decision of the attending physician. Doses were calculated by treatment planning software Xio 4.80 (Elekta AB). Treatment planning system (TPS) is calibrated in physical Gy. Prescription in GyE was recalculated by factor of 1.1 from physical Gy. One or two irradiation fields were used depending on the PTV size and location. Single Field Uniform Dose (SFUD) approach was used when possible, otherwise intensity modulated proton therapy (IMPT) optimisation was used to achieve desired dose distribution, see Figure 2. Standard constraints for optimisation were used. Required tolerance doses were met. Only in the case of close proximity of tumour to cochlea or inner ear, the coverage of target volume was preferred to the detriment of dose load of those critical organs. Two oblique irradiation fields were used or one irradiation field with a 20% dose reduction at the distal edge of the field for the remaining 2 mm to compensate for higher RBE. Each plan underwent pre-treatment patient-related quality assurance (QA) by DigiPhant water phantom using a MatriXX PT (IBA Dosimetry, Schwarzenbruck, Germany) ionisation chamber array detector. Agreement between measured and calculated dose distribution for each field at 3 planes perpendicular to particular beam axis was evaluated by absolute gamma analysis. Planes were selected to represent whole irradiation situation – field entrance, centre of PTV and distal part of PTV. The gamma criteria of dose difference (DD) 3% and distance to agreement (DTA) 3 mm were used. A gamma score less than 1 for at least 95% of evaluation points was taken as threshold for accepting plan for treatment.

Enlarge this image.

Figure 2. Dose coverage using proton PBS.

Robustness of the treatment plans was not evaluated regularly. Due to experience, the positioning error at this anatomical area is very low so geometrical uncertainty is negligible.

Two orthogonal X-ray images were performed prior to each treatment session. The set-up position was evaluated according to bone structures, and the patient's position was adjusted using the robotic couch with 6° of freedom.

Control CTs were performed at 1- or 2-week intervals to check the position of structures and body surface. In the case of changes (e.g. change in paranasal cavities filling), quality assurance plans were prepared to evaluate the dose distribution changes. Replanning was triggered when the changes within the tumour or surrounding tissues led to a significant change in the planned dose distribution. Replanning was performed when the dose to critical organs was increased by more than 2 GyE or when the decrease in the coverage of PTV (PTV_D98%) was bigger than 2 GyE.

At the end of treatment, patients were followed up by their referring physician and annually by a radiation oncologist. Tumour size was assessed once a year by MRI scans. Toxicity was assessed according to the CTCAE scale version 4.⁷

All patients completed treatment without any interruption. The median follow-up is 42.2 months. Dosimetric parameters for individual plans are presented in Table 2.

Table 2 Dosimetric parameters for PTV and organs at risk for individual patients.

¹Patients with bilateral tumours.

Acute toxicity was mild in all patients. Nine of the 12 patients experienced mild skin erythema; no mucositis within the oral cavities was observed. Mild xerostomia was reported by 4 of the 12 patients, and two patients experienced temporary swallowing difficulty that did not required any treatment. Late toxicity (more than 3 months after radiotherapy) has so far been observed in one patient – ipsilateral ototoxicity with a 60% of hearing loss. The mean dose to cochlea was 21 GyE in this case. There is probably no correlation to dose and hearing loss in this case. Any other late toxicities have not been observed. Acute and late toxicity in individual patients is summarised in Table 3.

Table 3 Acute and late toxicity (CTCAE v.4 scale).

All patients remain alive at the time of evaluation. No changes in primary tumour size were observed on follow-up MRIs. Necrotic tumour changes were observed in one patient on a control MRI 24 months after radiotherapy. One patient with primary metastatic disease had progression of metastatic lesions in the lung and liver and received two cycles of peptide receptor radiotherapy (PRRT). This patient is now in partial remission. No worsening of symptoms was observed. Table 4 summarises treatment results.

Table 4 Treatment results for individual patients.

FU, follow-up; SD, stable disease.

Glomus jugulare tumours are rare tumours what make their optimal management unclear. Surgical treatment poses risks such as cranial nerve damage, leakage of cerebrospinal fluid and other postoperative complications – especially when dealing with larger tumours.^8–10 Since these tumours are benign with very slow growth and patients usually experience minimal symptoms, these surgical complications have become difficult to tolerate in recent years.

Radiotherapy is a viable alternative to surgery.¹¹ For instance, in reported treatment results for 88 glomus tumours in 66 patients receiving external radiotherapy with an average dose of 45 Gy/25 fractions (average GTV size was 30 cm³), the authors describe 100% tumour control at 5 years and 98.7% control at 10 years. Acute grade 3 toxicity requiring hospitalisation was reported in 13% of patients and late grade 3 toxicity such as carotid and middle cerebral artery stenosis and brain necrosis in 4.5% of patients. We noticed none of these complications.

An alternative to fractionated radiotherapy is stereotactic radiosurgery that can be performed using gamma-knife, cyber-knife or linear accelerators.⁵ In reported treatment results using SRT in 46 patients (with a median GTV size of 3.6 cm³ and median dose of 20 Gy), the authors achieved a 42% improvement in neurological deficit and a reduction in tumour size on follow-up imaging examinations in 42% of patients.¹² In the long-term results for gamma-knife radiosurgery in 75 patients with a median follow-up time of 51.5 months (and average tumour volume of 7 cm³ with an average dose of 18 Gy), authors described improvement of pre-existing deficits in 15 patients (20%) and stabilisation was noted in 48 patients (64%). Twelve patients (16%) had new symptoms or progression of their pre-existing symptoms, and the main factor associated with a higher risk of developing these complications was tumour size.¹³ Additionally in reported treatment results for 30 patients with GJT treated with stereotactic radiotherapy with linear accelerators (with a median follow-up time of 4.6 years, a mean tumour volume of 56 cm³ with a typical dose of 14 Gy in one fraction), authors described tumour control at 97% with long-term grade 1 toxicity at 13%.

Radiotherapy is therefore an alternative to surgery at more advanced stages (Fisch class C-labyrinth and petrous bone is affected and D-intracranial spreading).¹⁴ Radiotherapy has lower complication rates and similar or better local control rates in this cases.¹⁵ However, the follow-up period for radiosurgical series is no longer than 5 years – late and very late consequences of radiotherapy may occur through longer observed follow-up times. Fractionated radiotherapy is known to lead to the induction of secondary malignancies such as meningiomas.¹⁶ At present, there exists a lack of information about the possible induction of secondary malignancies after radiosurgery or stereotactic radiotherapy. Another potential complication is vascular damage leading to ischemia or cognitive dysfunction.^17,18 The higher incidence of stroke has not yet been published for SRT for meningiomas.¹⁹ However, follow-up time in this case remains insufficient to exclude this possibility. Furthermore, SRT or radiosurgery is not suitable for large tumours near the brainstem or other critical structures. Volume limits for SRT are not clearly given but range from 10 to 25 cm⁶.²⁰ All of the above complications are dose-dependent, and their development involves in particular medium and low doses applied to large volumes of healthy tissue. Proton radiotherapy with pencil-beam scanning technology reduces these low-dose bath problems due to a finite range within the tissue. GJTs are usually located laterally, and this localisation maximises the benefit of finite range of protons for radiotherapy. Likewise, this solves the problem of radiotherapy for large tumours since protons have no GTV size limitations.

Due to the very low incidence of GJT and the poor availability of proton therapy, data on the effects of proton therapy are seriously lacking. In fact, the use of proton radiotherapy is described in only one case of glomus tumour.²¹ Our retrospective series includes patients with large tumours unsuitable for surgery or stereotactic radiotherapy. Dosimetric parameters demonstrate that even for large tumours treated with proton therapy the dose to critical organs can be significantly reduced. Acute toxicity is minimal and long-term toxicity additionally remains minimal. At time of writing, no patient has developed tumour progression within the treated area. To the best of our knowledge, this is the largest group of patients treated to date with proton beam therapy for GJT. Due to low number of cases and low incidence of events, survival and incidence analysis was not performed. This is a limitation of this study and can be addressed in future studies.

The disadvantage of the study is its retrospective nature, a small number of patients and its short follow-up time. The use of PBS in the treatment of GJT needs a larger patient group and a longer follow-up period. However, in the case of large tumours unsuitable for SRT using of PBS should be considered.

Proton pencil-beam scanning radiotherapy is feasible in the treatment of large GJT with mild acute toxicity and promising short-term results. The use of PBS appears to be particularly encouraging for younger patients with a long-life expectancy.

This work was supported by the European Regional Development Fund-Project: ‘Engineering Applications of Microworld Physics’ (No. CZ.02.1.01/0.0/0.0/16_019/0000766).

None declared.

The study was approved by Proton Therapy Centre institutional ethics committee and was conducted according to local ethical standards. All patients signed informed consent with the treatment before inclusion to the clinical registry.