Medical and microbiology records of seventeen patients (17 eyes), diagnosed as scleritis of infectious origin were reviewed; to study clinical features, predisposing risk factors, microbiologic profile and treatment outcome of infectious scleritis. The mean patient age was 52.3±19.75 years. Twelve patients (70.6%) had history of trauma/prior surgery. Isolated organisms included Staphylococcus species (spp) (n=5), Fungus (n=4), Nocardia spp (n=3), two each of atypical Mycobacterium spp and Streptococcus pneumoniae and one Pseudomonas aeruginosa. Treatment included intensive topical antimicrobial in all eyes and systemic medication in 15 (88.2%) patients; surgical exploration was needed for 13 (76.5%) patients and scleral patch graft was done in four (23.5%) patients. Lesions resolved in all patients and none required evisceration. The presenting log MAR visual acuity of 1.77±1.40 and improved to 0.99±0.91. (P≤0.039) after treatment with a mean follow up of 22.57±19.53 weeks. A microbiological confirmation, appropriate medical and/or surgical intervention has a good tectonic and visual outcome.
1. Introduction
Infectious scleritis presents as an ulcerated or nonulcerated, inflamed scleral nodule [1]. It accounts for 5–10% of all cases of scleritis [2–5]. But the presenting picture of infectious scleritis may not differ too much from immune-mediated scleritis [6–10]. Approximately 40–90% of immune mediated scleritis have an associated systemic vascular disease [3, 4, 6, 10]. While systemic treatment with corticosteroids or immunosuppressant benefits immune-mediated scleritis, it worsens the infectious scleritis. Hence it is imperative to differentiate between two conditions.
Many authors have reported infection by Pseudomonas aeruginosa and fungus as the most common causative organism [1, 11–13]. Pterygium surgery with beta radiation or application of mitomycin C has been identified as a common risk factor for infectious scleritis [11–13].
The clinical outcome is generally poor and most cases required evisceration in the many series [8, 9, 14]. Systemic and topical medication combined with early surgical intervention have improved the anatomical success, but not the visual outcome in two other series [1, 12].
Infectious scleritis is a rare entity; hence it is not suspected at the initial presentation resulting in delayed diagnosis and treatment. In this communication, we describe the predisposing factors, clinical features, etiology, and treatment outcome of infectious scleritis.
2. Material and Method
We retrospectively reviewed the medical and microbiological records of all patients with microbiologically proven infectious scleritis examined at Cornea Services of L V Prasad Eye Institute Bhubaneswar from November 2006 to August 2009. At presentation, all patients had received a detailed ophthalmic examination in the office. Patients with ulcerative lesions had received a scraping with a no. 15 surgical blade on a Bard Parker handle from the base and active edges of the ulcer under topical anesthesia in the office, and all nonulcerative nodular abscesses had received scleral scraping in the operating room under peribulbar anesthesia. In the later case, the base of the lesion was scrapped after dissecting the conjunctiva and deroofing of the nodular lesion. Materials collected from the lesions were smeared on glass slides and stained with Potassium hydroxide + Calcoflour white stain, Grams stain, Zeihl Neelsen stain using 20% H2SO4 or modified Zeihl Neelsen stain using 1% H2SO4. Acid fast staining was usually done if Grams stain smear was negative, but the lesions were strongly suspicious of microbial origin. The exudates from the lesion were cultured on blood agar, chocolate agar, Sabouraud’s dextrose agar (SDA), Brain-heart infusion broth and non-nutrient agar with an Escherichia coli overlay. All media were incubated at 37°C except SDA; this was incubated at 27°C. Significant growth was defined as confluent growth on solid media, and/or there was growth of the same organism on more than one medium, and/or growth in one medium was accompanied by presence of similar organism in smears. All bacteria and fungi grown were identified as per standard protocol, and bacteria were tested for antibiotic susceptibility by Kirby-Bauer disc diffusion method.
The initial therapy either was based on results of smear or when smear was negative, an empirical treatment with topical antibiotic (mostly gatifloxacin 0.3% and amikacin 2.5%) along with systemic gatifloxacin ((400 mg) twice daily) was given. The treatment was modified, if needed, based on final culture and sensitivity report. Surgical debridement was done should the scleral ulceration area extend locally or progressed to form a subconjunctival abscess at another site away from the main lesion.
The collected retrospective data included patient demography (age, gender, occupation), disease history (onset, course, predisposing factors), clinical feature, type of organisms, antibiotic susceptibility, treatment given, and the outcome.
3. Results
We included 17 patients (17 eyes) of infectious scleritis between November 2006 and August 2009. The inclusion criteria were presentation with a scleral ulcer and/or abscess and an organism isolated microbiologically. This included 7 women and 10 men; the age ranged from 13 years to 75 years (mean 52.3 ± 19.75 years, median 55 years). (Table 1) The mean followup was 22.57 ± 19.53 weeks (range of 3–89 weeks).
Patient demographic, clinical, and microbiological feature, management, and outcome.
Sl. no.
Age
Sex
Eye
History
Duration of symptoms (in days)
Presenting visual acuity
Clinical signs
Organism
Treatment
Final visual acuity
Remarks
Outcome
Topical
Systemic
Surgical
1.
72
M
OS
Cataract surgery
45
CF 2 m
Necrosis, corneal infiltrate
S. aureus
F. cefazolin, ciprofloxacin
Ciprofloxacin
TA + BCl
20/70
Corneal scar
Resolved
2.
65
M
OD
Nil
60
20/40
Abscess
Nocardia spp.
F. amikacin, gatifloxacin
TMX-SMZ
Exploration-2
20/60p
Cataract
Resolved
3.
19
F
OS
Nil
150
20/25
Punched out ulcer
Atypical mycobacterium
F. amikacin, ciprofloxacin
TMX-SMZ, prednisolone
Nil
20/30
Corneal infiltrate, choroidal
Resolved
4.
72
M
OS
Cataract surgery
45
CF 2 m
Necrosis
Fusarium spp.
Natamycin, gatifloxacin, cyclosporine
Itraconazole
SPG
20/120
Graft vascularized
Resolved
5.
35
F
OD
Injury (with stick)
15
CF 2 m
Abscess, corneal infiltrate
Fungus
Natamycin, gatifloxacin
Itraconazole
Exploration, Intracameral ampho- B
20/160
Corneal scar and cataract
Resolved
6.
66
M
OD
Cataract surgery
9
HM
Scleral necrosis, exudate
S. pneumoniae
F. cefazolin, gatifloxacin, betamethasone
Lizolidine, predinisolone
SPG + IOAB
20/60
Graft vascularized
Resolved
7.
49
M
OD
Nil
120
20/20
Ulcer, abscess, thinning
Staphylococcus spp.
Ciprofloxacin, prednisolone
Prednisolone
Nil
20/20
Nil
Resolved
8.
50
M
OS
Cataract surgery
7
HM
Necrosis
S. aureus
F. cefazolin, ciprofloxacin
Gatifloxacin
SPG + Vitreous biopsy + IOAB
20/100
Graft vascularized, corneal scar
Resolved
9.
74
F
OS
Injury (with mud)
15
HM
Abscess
P. aeruginosa
F. amikacin, Ciprofloxacin, Prednisolone
Ciprofloxacin, prednisolone
Exploration
20/200
Cataract, choroidal
Resolved
10.
50
F
OD
Injury (with twig)
75
20/30
Chemosis, abscess
Nocardia spp.
F. amikacin, ciprofloxacin
Ciprofloxacin
Exploration SPG + AMG
20/20
Graft vascularized
Resolved
11.
13
M
OD
Trabeculectomy
30
CF 1 m
Abscess
S. aureus
F. cefazolin, gatifloxacin
Cefadroxil
Nil
CF 1 m
Glaucoma, optic atrophy
Resolved
12.
21
M
OS
Thyroid Ophthalmoplegia
Not available
20/20
Abscess
S. pneumoniae
F. gentamicin, chloramphenicol
Prednisolone
Nil
20/30
Nil
Resolved
13.
53
M
OS
Retinal detachment surgery (buckle)
60
CF 1 m
Ulcer, abscess
Atypical mycobacterium
F. amikacin, gatifloxacin
Gatifloxacin
BB Removal
HM
Elevated Granuloma
Resolved
14.
55
F
OS
Nil
60
20/200
Thinning, ulcer, abscess
Nocardia spp.
F. amikacin, ciprofloxacin
Ciprofloxacin, TMX-SMZ
Exploration-3
20/50
Nil
Resolved
15.
75
F
OD
Cataract surgery
60
HM
Necrosis
Fungus
Natamycin
Itraconazole
TA + BCL
20/50
Corneal scar
Resolved
16.
65
F
OS
Cataract surgery
7
20/70
Necrosis, corneal infiltrate
S. aureus
F. cefazolin, gatifloxacin, prednisolone
Ciprofloxacin
Wound repair + IOAB
20/40
Membrane over IOL
Resolved
17.
55
M
OS
Cataract surgery
30
20/160
Necrosis
Paecilomyces spp.
Natamycin
Ketoconazole
SPG
PL+
Pupillary membrane
Resolved
The most common predisposing factor was an ocular surgery [n=9; 52.9%. 95% (CI), 29.27–76.73]. The surgery included cataract in seven eyes, scleral buckle in one eye, and trabeculectomy in one eye. The interval from surgery to diagnosis of infectious scleritis ranged from one week to four years. Four patients had injury with organic material like wood and mud three weeks to seven months prior to presentation (mean 37 ± 33.04 days; median 21 days). Fifteen of 17 patients were using topical corticosteroids and two patients were using oral corticosteroids at the time of reporting to us. Only one patient was diabetic in this series.
The symptoms present in all patients were redness, pain, and watering in the affected eye. The presenting visual acuity varied from hand motions (HM) to a normal vision of 20/20. Twelve patients (70.54%) presented with a vision less than 20/40. Unifocal or multifocal scleral abscess was seen in six patients (35.39%) (Figures 1(a) and 1(b)). Characteristically, the abscesses presented as yellowish nodules under the intact conjunctival epithelium. Scleral ulceration and necrosis was seen in eight patients (47.05%) (Figures 1(c) and 1(d)). Necrosis around the incisional area was seen in all seven patients who had received cataract surgery earlier. Three eyes (17.34%) had both ulceration and abscess (Figure 2(a)).
Slit lamp picture depicting different clinical presentation. (a) Case no. 2: multiple scleral abscess. (b) Case no.12: single scleral abscess. (c) Case no. 4: necrotic ulcer (post cataract surgery). (d) Case no. 3: two punched out ulcers.
Slit lamp picture of Case no. 10. (a) At Presentation showing multiple abscesses and ulcer. (b) Three weeks after initiation of treatment (surgical exploration and medical management), there is a uveal show. (c) Final outcome showing vascularized scleral graft (four months after scleral patch graft).
The culture grew a variety of organisms. They included Staphylococcus species (n=5; 29.41%), fungus (n=4; 23.52%), Nocardia species (n=3; 17.6%), Streptococcus pneumoniae (n=2), atypical Mycobacterium (n=2), and Pseudomonas aeruginosa (n=1). One of the four Staphylococcus was methicillin resistant (no. 7). Of the four fungi isolated, two could not be identified, one belonged to Fusarium and Paecilomyces species each.
The results of antibiotic susceptibility testing for bacterial isolates (Kirby Bauer disc diffusion method) are given in Table 2. Staphylococcal and streptococcal cases were treated with fortified Cefazolin (50 mg/mL) and a flouroquinolone (ciprofloxacin 0.3%/gatifloxacin 0.3%) along with systemic fluoroquinolones (ciprofloxacin 500 mg/gatifloxacin 400 mg twice daily). Patient no. 7 was treated only with topical ciprofloxacin. Fungal scleritis was treated with topical natamycin 5% and systemically either itraconazole (100 mg) or ketoconazole (200 mg) two times daily. Nocardia and atypical Mycobacterium scleritis were treated primarily with topical fortified amikacin (25 mg/mL). Systemic trimethoprim (160 mg) sulphamethoxazole (800 mg) (TMX-SMZ) combination was used in patients of Nocardia scleritis only.
Results of antibiotic susceptibility testing for bacterial isolates (Kirby Bauer disc diffusion method).
Thirteen of the 17 patients underwent wound debridement. During the surgical debridement, it was noticed that the area actually involved was generally much larger than initially seen under slit lamp. N-Butyl Cyanoacrylate glue was used in two patients as there was a limbal perforation of less than 1 mm × 1 mm in size. Five patients received scleral patch graft; as primary procedure in one (patient no. 4, Figure 1(c)), and the remaining four eyes, 2 days to one month after initiation of medical treatment. Seven eyes needed multiple surgical interventions.
Oral corticosteroid (1 mg/kg of body weight) was used in 5 eyes with bacterial scleritis two days after antibacterial treatment. In case no. 4, scleral patch graft was done as the primary procedure, later fungal filaments were identified from smear; so corticosteroids were started only after two weeks when recurrence was not noticed. Intraocular antibiotic was used in three patients suspected to have endophthalmitis. All of them presented scleral infection after cataract surgery.
Resolution was defined as absence of symptoms, congestion, or active infiltrate. All the patients in this series responded to treatment; 13(76.47%) patients had only scarring with no or minimal uveal show; one patient required scleral patch graft (Patient no. 10 Figures 2(a), 2(b), and 2(c)) one month after initiation of treatment. In the patients where scleral patch graft was done, success was defined as no evidence of graft or surrounding infiltrate and vascularization of the graft. All five grafts were healthy at the last visit.
The mean presenting and post treatment logMAR visual acuity was 1.77 ± 1.40 and 0.99 ± 0.91. (P≤0.039) (Figure 3). The vision improved by greater than 2 lines in 8 of 12 patients who presented with a visual acuity of <20/40 patients.
Comparision of the presenting visual acuity with posttreatment logMAR visual acuity of all patients.
The primary cause of decreased vision after resolution of infection was cataract and corneal scar. Total choroidal detachment developed in two patients and was treated with tapering oral corticosteroids. One of the two patients had atypical Mycobacteria infection. This 19-year-old lady also developed a corneal abscess after seven months of treatment. It resolved with topical fortified amikacin.
4. Discussion
Scleritis may represent a diagnostic challenge and is often associated with life-threatening systemic disease (in this series, only one patient had diabetes mellitus though) and vision-threatening ocular complications [15].
Scleral infection from Pseudomonas, Staphylococcus, or Herpes zoster virus can cause necrotizing scleritis, which is clinically identical to systemic autoimmune disease [6]. Unusual organisms like Nocardia, Acanthamoeba, atypical Mycobacteria, Mycobacterium tuberculosis, and Listeria monocytogenes are known to cause scleritis [1, 16–18]. Often the diagnosis of an associated infection or systemic condition dictates therapy. Systemic vasculitis typically requires systemic corticosteroid or immunosuppressive drugs [2, 3]. An early and definitive diagnosis helps in treatment of the condition and has better outcome.
Patients with a history of prior ocular surgery or trauma and presenting with a scleral abscess or ulceration and necrosis should arouse the suspicion of infectious origin. The surgeries include pterygium, cataract, scleral buckling, and strabismus surgery [10–12, 18]. In our series, cataract surgery was the predisposing factor in seven eyes and trauma with organic material was present in four eyes.
Corticosteroids, given before infection control, in an infectious scleritis worsen the condition by inhibiting release of lysosomal enzyme. In this cohort, 15 of 17 patients were on topical corticosteroids at presentation to us. It is unknown whether this aggravated the infection or decreased the immunity for secondary infection to occur.
Bacterial infectious scleritis is more common than other infectious scleritis. P. aeruginosa has been the often reported infecting organism [10, 12, 13, 15]. It was reported in over 50% eyes from Taiwan following pterygium surgeries [12, 13]. In our cohort, however, Staphylococcus infection (24.41%) and cataract were the most common surgery (41.17%). In our series, only one of 17 patients had P. aeruginosa infection.
One of our coauthors has reported fungal infectious scleritis in over one of third patients and high incidence of Nocardia infection from Hyderabad (south central India) [1]. In this series, we detected fungus in close to a quarter of patients and Nocardia in close to 20 percent. High incidence of fungus in both series can be attributed to the hot and humid climate and the enormous amount of fungal spore prevalent in the environment [19]. Two of the three patients with Nocardia scleritis could not recollect any history of injury although one of them was an agriculturist. All three patients with Nocardia scleritis required multiple explorations of the abscess, and one patient (no. 10) (Figures 2(a), 2(b), and 2(c)) required a scleral patch graft after resolution of the active infection.
In addition to topical medications, systemic antibiotic or antifungal was required for 15 patients. Systemic corticosteroids were used in patients with bacterial infection (n=5), in eyes that developed choroidal detachment (n=2), and in the patient who developed exophthalmous (no. 12).
Pyogenic infections of the sclera are often difficult to eradicate because of poor antimicrobial penetration into the avascular necrotic sclera; combination of surgery such as abscess exploration and systemic and topical antimicrobial therapy yields superior results [1, 13, 20, 21]. Surgical debridement not only facilitates penetration of antibiotic but also debulks the infected scleral tissue.
We do agree with Lin et al. who suggested mandatory surgical exploration of the abscess that does not respond to initial medication to increase the penetration of antibiotic [13]. Raber et al. reported a “tunnel lesion” on histopathological finding in cases of scleral ulcer [22]. Our experience is similar to Lin et al. who also described the tunnel lesion and recommended the need of careful exploration to avoid residual infection [13]. Two (no. 2, 14) of our 7 patients in this series required multiple surgical intervention and both of them had “tunnel lesion”.
All 17 patients in this series achieved anatomical success. Fourteen of 17 patients (82.35%) regained useful vision (defined as vision ≥20/200). The causes of poor vision in the remaining three eyes were glaucomatous optic atrophy (no. 11), chronic retinal detachment (no. 13), and fibrotic membrane in the pupillary area (no. 17). In an earlier series by one of our coauthors, one-third of patients had regained useful vision, but three of 21 eyes were eviscerated and one eye became phthisical [1]. Eleven of the 18 eyes in Hsiao et al. series retained useful vision, three had poor vision and four had to be eviscerated [12]. None of our patients in this series required evisceration.
Associated uveitis is not uncommon. (66% in Su et al. series) These inflammations lead to formation of pupillary membrane, cataract, and endophthalmitis [10]. Most patients in our series had low-grade inflammation in the anterior chamber at presentation; severe intraocular inflammation occurred in five patients subsequently. Cataract was the most common sequel in our series (n=3). Four patients who had extension to cornea resolved with corneal scar.
Our series has all weaknesses inherent to all retrospective studies. Our institution is a tertiary care referral center, so there is a potential for bias towards more unusual or difficult-to-control diseases. Nonetheless, we have demonstrated that a variety of organism can cause scleritis. An early clinical suspicion of infectious origin, identification of the infecting organism, knowledge of antibiotic susceptibility, and institution of appropriate medical and/or surgical therapy could have good tectonic and visual outcome.
Conflict of interests
The authors declare no conflict of interests.
Acknowledgment
The authors would like to thank Hyderabad Eye Research Foundation for support.
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