Background
Choroidal hemangioma is a benign, relatively rare vascular hamartoma that can present as a solitary, isolated lesion: circumscribed choroidal hemangioma (CCH), and less frequently, as an extensive lesion associated with Sturge-Weber syndrome: diffuse choroidal hemangioma1,2. Typically, CCH is seen as a discrete, smooth, round or oval, orange-red mass in the posterior pole with relation to the macular or peripapillary area3. On fluorescein angiography (FA), an early, diffuse hyperfluorescence is characteristic, whereas high to medium internal reflectivity on ultrasonography (US) is typical2. According to location and anatomic characteristics, a patient can be asymptomatic or present severe visual impairment3. Chronic subretinal fluid exudation from the tumor may result in serous retinal detachment (SRD), the principal cause of visual loss in these patients4.
Therapeutic measures are indicated when visual acuity (VA) decreases5. According to the current evidence, the use of photodynamic therapy (PDT) as the first-line treatment in patients with SRD can achieve tumor regression with visual improvement and/or stabilization1,4,6-8. We report the case of a successfully treated case of CCH with PDT as monotherapy and the anatomical changes during follow-up imaged with optical coherence tomography (OCT).
Clinical Case
A 70-year-old male with no relevant medical history presented to our outpatient ophthalmology clinic with a 3-week history of blurred vision, visual distortion, and referring a positive scotoma in the central visual field of the left eye. His best-corrected VA (BCVA) was of 20/60 for the right eye (OD) and 20/160 for the left eye (OS). Automated refraction revealed sphere (SPH) −3.75 and cylinder (CYL) −1.25 for OD, and SPH +3.50 and CYL −1.00 for OS.
Anterior segment biomicroscopy revealed nuclear cataract in both eyes (OU) (nuclear opalescence grade 2 and nuclear color grade 2, according to the lens opacity classification score III) that did not correlate with the patient's VA of OS. The rest of the anterior segment examination was unremarkable OU. Intraocular pressure was 10 mmHg OU. On posterior segment, examination under mydriasis of OS an isolated, oval, yellow-orange, and mottled elevated lesion of approximately 3 disc diameters with an associated SRD was identified in the temporoinferior macular area (Fig. 1A). Clinical diagnosis of CCH was made and confirmed with FA and OCT (Fig. 1, B through F). On FA, a typical early hyperfluorescence with large vascular spaces and late staining was evidenced (Fig. 1D-E). OCT detailed SRD, revealed a vitreomacular traction (VMT) syndrome (Fig. 1B), and confirmed the anatomy of the dome-shaped tumor on the temporal aspect of the macula (Fig. 1C).
Following informed consent, and after discussing with the patient the current treatment modalities, a session of PDT with verteporfin (Visudyne, Novartis Ophthalmics AG, Basel, Switzerland) at 6 mg/m2 body surface area consisting of three cycles was administered (exposure time of 83 s, laser light of 689 nm at an intensity of 600 mW/cm2, and radiant exposure of 50 J/cm2). A spot covering the totality of the tumor area was used. No adverse events such as discomfort, low back pain, chest pain, transient visual loss, catheter-induced complications, or photosensitivity were presented during or immediately after the procedure.
On follow-up, the patient was examined at day 5 after PDT reporting significant visual improvement (hereafter, BCVA refers to the affected eye). His BCVA was of 20/60 and an automated refraction revealed SPH +2.00 and CYL −0.75 OS. Posterior segment fundoscopy revealed an evident reduction of SRD, confirmed by OCT (Fig. 1G-I). On month 2 after PDT, the patient's BCVA remained stable at 20/60. On posterior segment, biomicroscopy atrophic and pigmentary changes were evidenced in the area of the CCH and macular OCT confirmed a complete retinal reattachment and evidenced VMT syndrome (Fig. 1J-L).
On year 1 of follow-up and after cataract surgery, our patient's BCVA was 20/25 despite VMT syndrome; BCVA remained stable up to year 2 (Fig. 2 A-B). A discussion with detailed explanation of the available surgical procedures was carried out with the patient and the decision to continue his management conservatively was made.
Discussion
The use of PDT proved to be an excellent monotherapy in our patient with CCH, achieving significant visual and anatomic improvement. Diagnosis of CCH is made clinically and presents as a solitary round-oval, red-orange, elevated lesion in the parapapillary or macular area9. Despite being the 3rd decade of life the most frequent age of diagnosis, our patient was diagnosed in his 8th decade of life. Relevant differential diagnoses are posterior scleritis, central serous chorioretinopathy, wet age-related macular degeneration, retinoblastoma, choroidal metastases, and amelanotic melanoma1.
The treatment of symptomatic CCH includes techniques such as laser photocoagulation, cryotherapy, brachytherapy, proton beam radiation, and transpupillary thermal therapy1,3,4. These modalities of treatment achieve tumor obliteration by producing tissue destruction with chorioretinal scarring/atrophy that results in unfavorable visual outcomes. Recurrences are common with these procedures3. The suitability of these techniques comes to question when the area of treatment involves the macula and/or is located near the fovea1,3,4. Theoretically, the use of PDT is the ideal method of treatment due to its selective destruction of endothelial cell membranes of the tumor vascular network and preservation of the overlying retinal cytoarchitecture8. A greater volume in the dilated vessels of the hemangioma could play a potentially relevant role increasing the selectivity and effectivity of the treatment5,10. As a result, PDT has become the first-line treatment for patients with macular CCH3,4.
PDT with verteporfin is administered at a dose of 6 mg/m2 of body surface area and exposure to a laser light dose of 689 or 692 nm at an intensity of 600 mW/cm2. The radiant exposure ranges from 50 to 100 J/cm2. There is no consensus about the treatment parameters. In a study made by Porrini et al.11, radiant exposure was titrated according to the height of the lesion. When the measured height was <2 mm, 75 J/cm2 with an exposure time of 125 s was used, and when the height was >2 mm, 100 J/cm2 with an exposure time of 186 s was implemented. In addition, some authors apply a single spot covering the entire lesion11,12, others use a spot to cover only the most prominent part of the tumor13 and others apply 1 or more overlapping spots14. The number of sessions ranges from 1 to 5, at intervals of 6-12 weeks1,3,11,13,15,16. In all studies, improvement or stabilization of VA, tumor flattening, or regression of macular edema was present as in our case. Our report is of a patient in which a darker iris and more choroidal pigmentation were present. Thus, the reaction to laser treatment is expected to be different than that of reports in different population. In accordance to this matter, parameters were individualized to protect the fovea, as described in the case presentation. Following treatment, anatomical and functional outcomes were positive: BCVA improved on the 1st week after PDT to 20/60, gained four lines of vision after cataract surgery (20/25), and remained stable thereafter despite VMT syndrome.
Cases were CCH becomes refractory to PDT or where repeated treatments are needed placing the eye at risk for chorioretinal ischemia still remain2. Incomplete destruction of the tumor vessels could play a role in this case, and as imaged in our patient, OCT-angiography (Fig. 2 C-D) proves to be a reliable method to assess the vascular cytoarchitecture of CCH. In our current era, where intravitreal antivascular endothelial growth factors (VEGF) have demonstrated to be effective and safe in treating chorioretinal neovascular and exudative conditions, their use as a treatment modality for CCH comes to mind. Kim et al.2 retrospectively evaluated the role of combination therapy of PDT + intravitreal bevacizumab in four eyes of a case series of 11. In this study, visual improvement was achieved in three of the eyes and one eye achieved visual stabilization. It is argued that anti-VEGF agents pose a synergistic effect with PDT, and that their use can be useful as adjuvant therapy to avoid the described decline in VA following PDT due to the rise in VEGF17, in parapapillary lesions that about the optic nerve3, and in patients with media opacities, overlying hemorrhage or cases with active exudation2.
Conclusion
Our report supports the safety and effectiveness of PDT as monotherapy in cases of CCH with macular involvement and SRD. It additionally provides evidence of possible safe parameters of PDT with verteporfin for eyes with darker irides and increased choroidal pigment content and documents OCT anatomical changes during time. We recommend the use of PDT with verteporfin as the first-line therapy and reserve the use of anti-VEGF for select cases in which PDT has proven insufficient or cases in which media opacities impede the correct application of the laser. Clinical trials in our population are needed to precisely characterize the effect of PDT and define the best treatment technique for each case.