A Pharmacodynamic Analysis of Choroidal Neovascularization in a Porcine Model Using Three Targeted Drugs

Tran, Justin; Craven, Caroline; Wabner, Kathy; Schmit, Jenn; Matter, Brock; Kompella, Uday B.; Grossniklaus, Hans E.; Olsen, Timothy W.

doi:10.1167/iovs.16-21230

Cited by 15 publications

(8 citation statements)

References 41 publications

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“…The rapid development of OCT technology since its inception in 1991 has provided exquisite methods to identify and evaluate multiple layers of the eye wall and eye tissue, including the vitreoretinal interface, retina, RPE, Bruch membrane, and choroid (Huang et al, 1991). The pig is being employed increasingly as a large animal model for experimental and preclinical studies for human diseases, including retinal vascular (Hein et al, 2012; Hein et al, 2010; Hein et al, 2016) and degenerative diseases (Mones et al, 2016; Scott et al, 2014), and choroidal neovascularization (Tran et al, 2017). Despite the widespread adoption of SD-OCT instrumentation in research laboratories, histologic correlation of the porcine retina with SD-OCT data remains limited.…”

Section: Discussionmentioning

confidence: 99%

Correlation of spectral domain optical coherence tomography with histology and electron microscopy in the porcine retina

Xie

Zhao

Tsai

et al. 2018

Experimental Eye Research

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Spectral domain optical coherence tomography (SD-OCT) is used as a non-invasive tool for retinal morphological assessment in vivo. Information on the correlation of SD-OCT with retinal histology in the porcine retina, a model resembling the human retina, is limited. Herein, we correlated the hypo- and hyper-reflective bands on SD-OCT with histology of the lamellar architecture and cellular constituents of the porcine retina. SD-OCT images were acquired with the Heidelberg Spectralis HRA + OCT. Histological analysis was performed using epoxy resin embedded tissue and transmission electron microscopy. Photomicrographs from the histologic sections were linearly scaled to correct for tissue shrinkage and correlated with SD-OCT images. SD-OCT images correlated well with histomorphometric data. A hyper-reflective band in the mid-to-outer inner nuclear layer correlated with the presence of abundant mitochondria in horizontal cell processes and adjacent bipolar cells. A concentration of cone nuclei corresponded to a relative hypo-reflective band in the outer portion of the outer nuclear layer. The presence of 3 hyper-reflective bands in the outer retina corresponded to: 1) the external limiting membrane; 2) the cone and rod ellipsoid zones; and 3) the interdigitation zone of photoreceptor outer segments/retinal pigment epithelium (RPE) apical cell processes and the RPE. These correlative and normative SD-OCT data may be employed to characterize and assess the in vivo histologic changes in retinal vascular and degenerative diseases and the responses to novel therapeutic interventions in this large animal model.

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Section: Discussionmentioning

confidence: 99%

Correlation of spectral domain optical coherence tomography with histology and electron microscopy in the porcine retina

Xie

Zhao

Tsai

et al. 2018

Experimental Eye Research

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“…Finally, the antibodies described herein could also be prioritized for the treatment of other diseases associated with upregulation of membranous TF expression, such as macular degeneration (49). A FVII-Fc fusion protein that binds TF reduces the size of choroid neovascular (CNV) lesions in various animal models (50,51). With the binding affinities of a subset of the anti-TF antibodies below the affinity of FVII for TF (52), some of the antibodies could be more efficacious than the FVII-Fc fusion protein.…”

Section: Discussionmentioning

confidence: 99%

Treating Tissue Factor–Positive Cancers with Antibody–Drug Conjugates That Do Not Affect Blood Clotting

Theunissen

Cai

Bhatti

et al. 2018

Molecular Cancer Therapeutics

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The primary function of tissue factor (TF) resides in the vasculature as a cofactor of blood clotting; however, multiple solid tumors aberrantly express this transmembrane receptor on the cell surface. Here, we developed anti-TF antibody-drug conjugates (ADC) that did not interfere with the coagulation cascade and benchmarked them against previously developed anti-TF ADCs. After screening an affinity-matured antibody panel of diverse paratopes and affinities, we identified one primary paratope family that did not inhibit conversion of Factor X (FX) to activated Factor X (FXa) and did not affect conversion of prothrombin to thrombin. The rest of the antibody panel and previously developed anti-TF antibodies were found to perturb coagulation to varying degrees. To compare the anticancer activity of coagulation-inert and -inhibitory antibodies as ADCs, a selection of antibodies was conjugated to the prototypic cytotoxic agent monomethyl auristatin E (MMAE) through a protease-cleavable linker. The coagulation-inert and -inhibitory anti-TF ADCs both killed cancer cells effectively. Importantly, the coagulation-inert ADCs were as efficacious as tisotumab vedotin, a clinical stage ADC that affected blood clotting, including in patient-derived xenografts from three solid tumor indications with a need for new therapeutic treatments-squamous cell carcinoma of the head and neck (SCCHN), ovarian, and gastric adenocarcinoma. Furthermore, a subset of the anti-TF antibodies could also be considered for the treatment of other diseases associated with upregulation of membranous TF expression, such as macular degeneration. .

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“…SCS delivery can result in high bioavailability in the sclera, choroid, and RPE[28, 32, 36, 59, 61, 66, 68–70, 88, 89]. For example, a small molecule HIF-1 inhibitor injected into the SCS of rats distributed throughout the choroid and retina, and prevented choroidal neovascularization in an animal model with selective destruction of Bruch’s membrane[69].…”

Section: Pharmacodynamicsmentioning

confidence: 99%

“…No studies have yet used SCS delivery for therapeutic effect on the RPE. Studies have shown that choroidal neovascularization is more effectively treated with intravitreal injections of a receptor tyrosine kinase inhibitor than SCS injections, although the authors noted incomplete delivery with the SCS injection[89]. …”

Section: Pharmacodynamicsmentioning

confidence: 99%

The suprachoroidal space as a route of administration to the posterior segment of the eye

Chiang

Jung

Prausnitz

2018

Advanced Drug Delivery Reviews

102

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The suprachoroidal space (SCS) is a potential space between the sclera and choroid that traverses the circumference of the posterior segment of the eye. The SCS is an attractive site for drug delivery because it targets the choroid, retinal pigment epithelium, and retina with high bioavailability, while maintaining low levels elsewhere in the eye. Indeed, phase III clinical trials are investigating the safety and efficacy of SCS drug delivery. Here, we review the anatomy and physiology of the SCS; methods to access the SCS; kinetics of SCS drug delivery; strategies to target within the SCS; current and potential clinical indications; and the safety and efficacy of this approach in preclinical animal studies and clinical trials.

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A Pharmacodynamic Analysis of Choroidal Neovascularization in a Porcine Model Using Three Targeted Drugs

Cited by 15 publications

References 41 publications

Correlation of spectral domain optical coherence tomography with histology and electron microscopy in the porcine retina

Correlation of spectral domain optical coherence tomography with histology and electron microscopy in the porcine retina

Treating Tissue Factor–Positive Cancers with Antibody–Drug Conjugates That Do Not Affect Blood Clotting

The suprachoroidal space as a route of administration to the posterior segment of the eye

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