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2015

Grob S, Jakobiec F, Stagner A, Colby K. Diffuse Epibulbar Complex Lacrimal-Cartilaginous Choristoma: Diagnostic Clues and Management.. Cornea. 2015;34(10):1321–3.

PURPOSE: To describe the clinical and histopathologic features distinguishing an extensive complex choristoma of the epibulbar surface and to address the management of such lesions. METHODS: Clinical history, diagnostic imaging studies, and histopathologic sections stained with hematoxylin and eosin were reviewed from a 2-year-old girl with a congenital conjunctival lesion of the right eye that was surgically excised. RESULTS: The patient clinically displayed an extensive, vascularized amelanotic conjunctival lesion located superotemporally with extension onto the cornea. Her visual acuity was reduced to 20/670. The clinical diagnosis was a large lacrimal gland choristoma with corneal involvement and resulting deprivation amblyopia. The patient underwent an excision of the lesion including the corneal portion, and the ocular surface was reconstructed with amniotic membrane. Histopathologic evaluation disclosed lobules of lacrimal tissue and cartilage plaques, smooth muscle, and nerves consistent with a complex choristoma. Six weeks postoperatively, the visual acuity had improved to 20/180. The patient returned to her local ophthalmologist for amblyopia management. CONCLUSIONS: We emphasize the importance of recognizing lesion-induced amblyopia and the timely performance of appropriate surgery for complex epibulbar choristomas. A differential diagnosis of other congenital epibulbar lesions is provided.

Lim LS, Ng WY, Wong D, Wong E, Yeo I, Ang CL, Kim L, Vavvas D, Lee SY. Prognostic factor analysis of vitrectomy for myopic foveoschisis.. Br J Ophthalmol. 2015;99(12):1639–43.

PURPOSE: To describe the anatomical and functional outcomes in a cohort of subjects undergoing vitrectomy for myopic foveoschisis, and to analyse the factors predicting foveal reattachment and visual improvement. METHODS: This retrospective case series evaluated case records and optical coherence tomography images 6 months after surgery. Multivariate linear and logistic regressions were performed to assess the factors predicting anatomical and visual improvement. RESULTS: In total, 55 eyes of 54 patients were analysed. The mean spherical equivalent refraction was -11.83±4.94D. Foveal detachment was present in 63.5% of eyes preoperatively and subjects with foveal detachment had 0.70 logMAR units (95% CI 0.02 to 1.39) poorer visual acuity than subjects without (p=0.046). The mean preoperative visual acuity was 0.84±0.59 logMAR units and the mean postoperative visual acuity was 0.64±0.64 logMAR units (mean difference 0.20±0.68 logMAR units (p=0.04)). The proportion of eyes with foveal detachment was significantly lower after surgery (12.5%; p<0.001). However, the proportion of eyes with ellipsoid zone disruption was significantly higher after surgery (59.6% vs 34.0%; p<0.001). In multivariate analyses, the preoperative central foveal thickness significantly predicted postoperative visual improvement by two or more lines (OR 1.004 (95% CI 1.000 to 1.007), per μm increase; p=0.049). The presence of ellipsoid zone disruption preoperatively was associated with 0.96 logMAR (95% CI 0.2 to 1.72) poorer final acuity (p=0.02). CONCLUSIONS: Eyes with myopic foveoschisis with preoperative ellipsoid disruption and thinner central foveal thickness tend to have poorer visual outcomes. While current surgical manoeuvres are effective in reattaching the fovea, they may also cause iatrogenic injury to the photoreceptors.

Silva P, Aiello LP. Reply.. Retina. 2015;35(7):e37–8.
Wirostko B, Rafii M, Sullivan D, Morelli J, Ding J. Novel Therapy to Treat Corneal Epithelial Defects: A Hypothesis with Growth Hormone.. Ocul Surf. 2015;13(3):204–212.e1.

Impaired corneal wound healing that occurs with ocular surface disease, trauma, systemic disease, or surgical intervention can lead to persistent corneal epithelial defects (PCED), which result in corneal scarring, ulceration, opacification, corneal neovascularization, and, ultimately, visual compromise and vision loss. The current standard of care can include lubricants, ointments, bandage lenses, amniotic membranes, autologous serum eye drops, and corneal transplants. Various inherent problems exist with application and administration of these treatments, which often may not result in a completely healed surface. A topically applicable compound capable of promoting corneal epithelial cell proliferation and/or migration would be ideal to accelerate healing. We hypothesize that human growth hormone (HGH) is such a compound. In a recent study, HGH was shown to activate signal transducer and activators of transcription-5 (STAT5) signaling and promote corneal wound healing by enhancing corneal epithelial migration in a co-culture system of corneal epithelial cells and fibroblasts. These effects require an intact communication between corneal epithelia and fibroblasts. Further, HGH promotes corneal wound healing in a rabbit debridement model, thus demonstrating the effectiveness of HGH in vivo as well. In conclusion, HGH may represent an exciting and effective topical therapeutic to promote corneal wound healing.

Aggarwal S, Kheirkhah A, Cavalcanti B, Cruzat A, Colón C, Brown E, Borsook D, Prüss H, Hamrah P. Autologous Serum Tears for Treatment of Photoallodynia in Patients with Corneal Neuropathy: Efficacy and Evaluation with InVivo Confocal Microscopy.. Ocul Surf. 2015;13(3):250–62.

OBJECTIVE: Patients suffering from corneal neuropathy may present with photoallodynia; i.e., increased light sensitivity, frequently with a normal slit-lamp examination. This study aimed to evaluate the efficacy of autologous serum tears (AST) for treatment of severe photoallodynia in corneal neuropathy and to correlate clinical findings with corneal subbasal nerve alterations by in vivo confocal microscopy (IVCM). METHODS: Retrospective case control study with 16 patients with neuropathy-induced severe photoallodynia compared to 16 normal controls. Symptom severity, clinical examination and bilateral corneal IVCM scans were recorded. RESULTS: All patients suffered from extreme photoallodynia (8.8±1.1) with no concurrent ocular surface disease. Subbasal nerves were significantly decreased at baseline in patients compared to controls; total nerve length (9208±1264 vs 24714±1056 μm/mm(2); P<.0001) and total nerve number (9.6±1.4 vs 28.6±2.0; P<.0001), respectively. Morphologically, significantly increased reflectivity (2.9±0.2 vs 1.8±0.1; P<.0001), beading (in 93.7%), and neuromas (in 62.5%) were seen. AST (3.6±2.1 months) resulted in significantly decreased symptom severity (1.6±1.7; P=.02). IVCM demonstrated significantly improved nerve parameters (P<.005), total nerve length (15451±1595 μm/mm(2)), number (13.9±2.1), and reflectivity (1.9±0.1). Beading and neuromas were seen in only 56.2% and 7.6% of patients. CONCLUSION: Patients with corneal neuropathy-induced photoallodynia show profound alterations in corneal nerves. AST restores nerve topography through nerve regeneration, and this correlated with improvement in patient-reported photoallodynia. The data support the notion that corneal nerve damage results in alterations in afferent trigeminal pathways to produce photoallodynia.

Joshi P, Esko T, Mattsson H, Eklund N, Gandin I, Nutile T, Jackson A, Schurmann C, Smith A, Zhang W, Okada Y, Stančáková A, Faul J, Zhao W, Bartz T, Concas MP, Franceschini N, Enroth S, Vitart V, Trompet S, Guo X, Chasman D, O’Connel J, Corre T, Nongmaithem S, Chen Y, Mangino M, Ruggiero D, Traglia M, Farmaki AE, Kacprowski T, Bjonnes A, Spek A, Wu Y, Giri A, Yanek L, Wang L, Hofer E, Rietveld C, McLeod O, Cornelis M, Pattaro C, Verweij N, Baumbach C, Abdellaoui A, Warren H, Vuckovic D, Mei H, Bouchard C, Perry J, Cappellani S, Mirza S, Benton M, Broeckel U, Medland S, Lind P, Malerba G, Drong A, Yengo L, Bielak L, Zhi D, Most P, Shriner D, Mägi R, Hemani G, Karaderi T, Wang Z, Liu T, Demuth I, Zhao JH, Meng W, Lataniotis L, Laan S, Bradfield J, Wood A, Bonnefond A, Ahluwalia T, Hall L, Salvi E, Yazar S, Carstensen L, Haan H, Abney M, Afzal U, Allison M, Amin N, Asselbergs F, Bakker S, Barr G, Baumeister S, Benjamin D, Bergmann S, Boerwinkle E, Bottinger E, Campbell A, Chakravarti A, Chan Y, Chanock S, Chen C, Chen I, Collins F, Connell J, Correa A, Cupples A, Smith GD, Davies G, Dörr M, Ehret G, Ellis S, Feenstra B, Feitosa M, Ford I, Fox C, Frayling T, Friedrich N, Geller F, Scotland G, Gillham-Nasenya I, Gottesman O, Graff M, Grodstein F, Gu C, Haley C, Hammond C, Harris S, Harris T, Hastie N, Heard-Costa N, Heikkilä K, Hocking L, Homuth G, Hottenga JJ, Huang J, Huffman J, Hysi P, Ikram A, Ingelsson E, Joensuu A, Johansson Å, Jousilahti P, Jukema W, Kähönen M, Kamatani Y, Kanoni S, Kerr S, Khan N, Koellinger P, Koistinen H, Kooner M, Kubo M, Kuusisto J, Lahti J, Launer L, Lea R, Lehne B, Lehtimäki T, Liewald D, Lind L, Loh M, Lokki ML, London S, Loomis S, Loukola A, Lu Y, Lumley T, Lundqvist A, Männistö S, Marques-Vidal P, Masciullo C, Matchan A, Mathias R, Matsuda K, Meigs J, Meisinger C, Meitinger T, Menni C, Mentch F, Mihailov E, Milani L, Montasser M, Montgomery G, Morrison A, Myers R, Nadukuru R, Navarro P, Nelis M, Nieminen M, Nolte I, O’Connor G, Ogunniyi A, Padmanabhan S, Palmas W, Pankow J, Patarcic I, Pavani F, Peyser P, Pietilainen K, Poulter N, Prokopenko I, Ralhan S, Redmond P, Rich S, Rissanen H, Robino A, Rose L, Rose R, Sala C, Salako B, Salomaa V, Sarin AP, Saxena R, Schmidt H, Scott L, Scott W, Sennblad B, Seshadri S, Sever P, Shrestha S, Smith B, Smith J, Soranzo N, Sotoodehnia N, Southam L, Stanton A, Stathopoulou M, Strauch K, Strawbridge R, Suderman M, Tandon N, Tang ST, Taylor K, Tayo B, Töglhofer AM, Tomaszewski M, Tšernikova N, Tuomilehto J, Uitterlinden A, Vaidya D, Hylckama Vlieg A, Setten J, Vasankari T, Vedantam S, Vlachopoulou E, Vozzi D, Vuoksimaa E, Waldenberger M, Ware E, Wentworth-Shields W, Whitfield J, Wild S, Willemsen G, Yajnik C, Yao J, Zaza G, Zhu X, BioBank Japan Project, Salem R, Melbye M, Bisgaard H, Samani N, Cusi D, Mackey D, Cooper R, Froguel P, Pasterkamp G, Grant S, Hakonarson H, Ferrucci L, Scott R, Morris A, Palmer C, Dedoussis G, Deloukas P, Bertram L, Lindenberger U, Berndt S, Lindgren C, Timpson N, Tönjes A, Munroe P, Sørensen T, Rotimi C, Arnett D, Oldehinkel A, Kardia S, Balkau B, Gambaro G, Morris A, Eriksson J, Wright M, Martin N, Hunt S, Starr J, Deary I, Griffiths L, Tiemeier H, Pirastu N, Kaprio J, Wareham N, Perusse L, Wilson J, Girotto G, Caulfield M, Raitakari O, Boomsma D, Gieger C, Harst P, Hicks A, Kraft P, Sinisalo J, Knekt P, Johannesson M, Magnusson P, Hamsten A, Schmidt R, Borecki I, Vartiainen E, Becker D, Bharadwaj D, Mohlke K, Boehnke M, Duijn C, Sanghera D, Teumer A, Zeggini E, Metspalu A, Gasparini P, Ulivi S, Ober C, Toniolo D, Rudan I, Porteous D, Ciullo M, Spector T, Hayward C, Dupuis J, Loos R, Wright A, Chandak G, Vollenweider P, Shuldiner A, Ridker P, Rotter J, Sattar N, Gyllensten U, North K, Pirastu M, Psaty B, Weir D, Laakso M, Gudnason V, Takahashi A, Chambers J, Kooner J, Strachan D, Campbell H, Hirschhorn J, Perola M, Polašek O, Wilson J. Directional dominance on stature and cognition indiverse human populations.. Nature. 2015;523(7561):459–62.

Homozygosity has long been associated with rare, often devastating, Mendelian disorders, and Darwin was one of the first to recognize that inbreeding reduces evolutionary fitness. However, the effect of the more distant parental relatedness that is common in modern human populations is less well understood. Genomic data now allow us to investigate the effects of homozygosity on traits of public health importance by observing contiguous homozygous segments (runs of homozygosity), which are inferred to be homozygous along their complete length. Given the low levels of genome-wide homozygosity prevalent in most human populations, information is required on very large numbers of people to provide sufficient power. Here we use runs of homozygosity to study 16 health-related quantitative traits in 354,224 individuals from 102 cohorts, and find statistically significant associations between summed runs of homozygosity and four complex traits: height, forced expiratory lung volume in one second, general cognitive ability and educational attainment (P < 1 × 10(-300), 2.1 × 10(-6), 2.5 × 10(-10) and 1.8 × 10(-10), respectively). In each case, increased homozygosity was associated with decreased trait value, equivalent to the offspring of first cousins being 1.2 cm shorter and having 10 months' less education. Similar effect sizes were found across four continental groups and populations with different degrees of genome-wide homozygosity, providing evidence that homozygosity, rather than confounding, directly contributes to phenotypic variance. Contrary to earlier reports in substantially smaller samples, no evidence was seen of an influence of genome-wide homozygosity on blood pressure and low density lipoprotein cholesterol, or ten other cardio-metabolic traits. Since directional dominance is predicted for traits under directional evolutionary selection, this study provides evidence that increased stature and cognitive function have been positively selected in human evolution, whereas many important risk factors for late-onset complex diseases may not have been.

Reddy A, Gonzalez M, Henry C, Yeh S, Sobrin L, Albini T. Diagnostic Sensitivity of Indocyanine Green Angiography for Birdshot Chorioretinopathy.. JAMA Ophthalmol. 2015;133(7):840–3.

IMPORTANCE: To describe a cohort of patients with birdshot chorioretinopathy who did not manifest birdshot lesions on clinical examination but had retinal vasculitis, low-grade to moderate vitritis, and hypocyanescent lesions on indocyanine green angiography (ICGA). OBSERVATIONS: Case series of 3 patients with mild to moderate vitritis and retinal vasculitis without definite birdshot lesions on clinical examination evaluated from January 2007 to December 2014 at 4 academic ophthalmology centers. All patients' results were positive for human leukocyte antigen-A29. All cases had hypocyanescent lesions visible on ICGA but not detectable on fluorescein angiography. CONCLUSIONS AND RELEVANCE: Patients with retinal vasculitis and low-grade vitritis with or without macular edema may have birdshot chorioretinopathy evident on ICGA before lesions are visible on clinical examination or fluorescein angiography. Expanding birdshot chorioretinopathy diagnostic criteria to include the presence of hypocyanescent lesions on ICGA could improve the sensitivity of diagnosis.

Rai R, Jakobiec F, Fay A. Ocular Metastatic Renal Carcinoma Presenting With Proptosis.. Ophthal Plast Reconstr Surg. 2015;31(4):e100–8.

Metastatic renal carcinoma is the third most common source of ocular and second most common source of orbital metastases. This is the first published case of von Hippel-Lindau (vHL) disease that developed renal cell carcinoma metastatic to an eye with a retinal hemangioblastoma. A 73-year-old woman had a history of vHL disease that included prior retinal hemangioblastomas, 2 cerebellar hemangioblastomas, and bilateral renal cell carcinomas with sacral metastasis. After presenting with progressive, painful proptosis secondary to a large mass observable by ocular CT, an enucleation-orbitotomy was performed, and the surgical specimen was sent for histopathological analysis. The ophthalmic renal metastatic tumor, like the primary tumor, was a clear cell variant that involved both the eyeball and orbit in continuity. The intraocular component was larger than the extraocular portion, which was interpreted as an outward extension of an initial retinal metastasis that probably first settled within a hemangioblastoma. Clusters of ectatic ghost vessels with thickened walls produced by periodic acid Schiff-positive, redundant basement membrane material were partially infiltrated by tumor cells at their periphery, thereby lending some support for this hypothesis. Immunohistochemical positivity for the biomarkers cytokeratin 18, vimentin, carbonic anhydrase IX, PAX2, and PAX 8 confirmed the diagnosis. The patient has refused further treatment. Her anophthalmic socket has comfortably retained a porous polyethylene implant without clinical evidence of local recurrence during 5 months of follow up.

Choi V, Bigelow C, McGee T, Gujar A, Li H, Hanks S, Vrouvlianis J, Maker M, Leehy B, Zhang Y, Aranda J, Bounoutas G, Demirs J, Yang J, Ornberg R, Wang Y, Martin W, Stout K, Argentieri G, Grosenstein P, Diaz D, Turner O, Jaffee B, Police S, Dryja T. AAV-mediated RLBP1 gene therapy improves the rate of dark adaptation in Rlbp1 knockout mice.. Mol Ther Methods Clin Dev. 2015;2:15022.

Recessive mutations in RLBP1 cause a form of retinitis pigmentosa in which the retina, before its degeneration leads to blindness, abnormally slowly recovers sensitivity after exposure to light. To develop a potential gene therapy for this condition, we tested multiple recombinant adeno-associated vectors (rAAVs) composed of different promoters, capsid serotypes, and genome conformations. We generated rAAVs in which sequences from the promoters of the human RLBP1, RPE65, or BEST1 genes drove the expression of a reporter gene (green fluorescent protein). A promoter derived from the RLBP1 gene mediated expression in the retinal pigment epithelium and Müller cells (the intended target cell types) at qualitatively higher levels than in other retinal cell types in wild-type mice and monkeys. With this promoter upstream of the coding sequence of the human RLBP1 gene, we compared the potencies of vectors with an AAV2 versus an AAV8 capsid in transducing mouse retinas, and we compared vectors with a self-complementary versus a single-stranded genome. The optimal vector (scAAV8-pRLBP1-hRLBP1) had serotype 8 capsid and a self-complementary genome. Subretinal injection of scAAV8-pRLBP1-hRLBP1 in Rlbp1 nullizygous mice improved the rate of dark adaptation based on scotopic (rod-plus-cone) and photopic (cone) electroretinograms (ERGs). The effect was still present after 1 year.