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Featured researches published by Howard Wessel.


Scientific Reports | 2017

Intranasal Delivery of A Novel Amnion Cell Secretome Prevents Neuronal Damage and Preserves Function In A Mouse Multiple Sclerosis Model

Reas S. Khan; Kimberly Dine; Bailey Bauman; Michael Lorentsen; Lisa Lin; Helayna Brown; Leah R. Hanson; Aleta L. Svitak; Howard Wessel; Larry R. Brown; Kenneth S. Shindler

The ability of a novel intranasally delivered amnion cell derived biologic to suppress inflammation, prevent neuronal damage and preserve neurologic function in the experimental autoimmune encephalomyelitis animal model of multiple sclerosis was assessed. Currently, there are no existing optic nerve treatment methods for disease or trauma that result in permanent vision loss. Demyelinating optic nerve inflammation, termed optic neuritis, induces permanent visual dysfunction due to retinal ganglion cell damage in multiple sclerosis and experimental autoimmune encephalomyelitis. ST266, the biological secretome of Amnion-derived Multipotent Progenitor cells, contains multiple anti-inflammatory cytokines and growth factors. Intranasally administered ST266 accumulated in rodent eyes and optic nerves, attenuated visual dysfunction, and prevented retinal ganglion cell loss in experimental optic neuritis, with reduced inflammation and demyelination. Additionally, ST266 reduced retinal ganglion cell death in vitro. Neuroprotective effects involved oxidative stress reduction, SIRT1-mediated mitochondrial function promotion, and pAKT signaling. Intranasal delivery of neuroprotective ST266 is a potential novel, noninvasive therapeutic modality for the eyes, optic nerves and brain. The unique combination of biologic molecules in ST266 provides an innovative approach with broad implications for suppressing inflammation in autoimmune diseases, and for preventing neuronal damage in acute neuronal injury and chronic neurodegenerative diseases such as multiple sclerosis.


Investigative Ophthalmology & Visual Science | 2018

RGC Neuroprotection Following Optic Nerve Trauma Mediated By Intranasal Delivery of Amnion Cell Secretome

Gabriela A. Grinblat; Reas S. Khan; Kimberly Dine; Howard Wessel; Larry R. Brown; Kenneth S. Shindler

Purpose Intranasally delivered ST266, the biological, proteinaceous secretome of amnion-derived multipotent progenitor cells, reduces retinal ganglion cell (RGC) loss, optic nerve inflammation, and demyelination in experimental optic neuritis. This unique therapy and novel administration route delivers numerous cytokines and growth factors to the eye and optic nerve, suggesting a potential to also treat other optic neuropathies. Thus, ST266-mediated neuroprotection was examined following traumatic optic nerve injury. Methods Optic nerve crush injury was surgically induced in C57BL/6J mice. Mice were treated daily with intranasal PBS or ST266. RGC function was assessed by optokinetic responses (OKRs), RGCs were counted, and optic nerve sections were stained with luxol fast blue and anti-neurofilament antibodies to assess myelin and RGC axon damage. Results Intranasal ST266 administered daily for 5 days, beginning at the time that a 1-second optic nerve crush was performed, significantly attenuated OKR decreases. Furthermore, ST266 treatment reduced damage to RGC axons and myelin within optic nerves, and blocked RGC loss. Following a 4-second optic nerve crush, intranasal ST266 increased RGC survival and showed a trend toward reduced RGC axon and myelin damage. Ten days following optic nerve crush, ST266 prevented myelin damage, while also inducing a trend toward increased RGC survival and visual function. Conclusions ST266 significantly attenuates traumatic optic neuropathy. Neuroprotective effects of this unique combination of biologic molecules observed here and previously in optic neuritis suggest potential broad application for preventing neuronal damage in multiple optic nerve disorders. Furthermore, results support intranasal delivery as a novel, noninvasive therapeutic modality for eyes and optic nerves.


Investigative Ophthalmology & Visual Science | 1997

Type XII Collagen Contributes to Diversities in Human Corneal and Limbal Extracellular Matrices

Howard Wessel; Susan C. Anderson; Dana Fite; Elias K. Halvas; John Hempel; Nirmala SundarRaj


Clinica Chimica Acta | 2004

Correlation of surrogate markers of Gaucher disease. Implications for long-term follow up of enzyme replacement therapy.

Mario A. Cabrera-Salazar; Erin O'Rourke; Nadene Henderson; Howard Wessel; John A. Barranger


Investigative Ophthalmology & Visual Science | 2000

Developmentally regulated appearance of spliced variants of type XII collagen in the cornea.

Susan C. Anderson; Sonali Sundarraj; Dana Fite; Howard Wessel; Nirmala SundarRaj


Investigative Ophthalmology & Visual Science | 1998

A Rho-associated protein kinase: differentially distributed in limbal and corneal epithelia.

Nirmala SundarRaj; Paul R. Kinchington; Howard Wessel; B Goldblatt; John R. Hassell; J P Vergnes; Susan C. Anderson


Archive | 2015

Methods for reducing and/or preventing excessive cellular apoptosis

Howard Wessel; Richard A. Banas


Investigative Ophthalmology & Visual Science | 2017

Anti-inflammatory effects of ST266, an amnion-derived multipotent progenitor cell-derived secretome, on corneal wound healing and stromal fibrosis in rabbits

Larry D. Brown; Howard Wessel; Erika Klitsch; Elise M. Gill; Justin Prater; David Culp; Brian C. Gilger; Kenneth J. Mandell


Investigative Ophthalmology & Visual Science | 2017

Anti-allergic effects of ST266, an amnion-derived multipotent progenitor cell-secretome, in ovalbumin-induced allergic conjunctivitis in guinea pigs

Kenneth J. Mandell; Howard Wessel; Erika Klitsch; David Culp; Justin Prater; Brian C. Gilger; Larry R. Brown


Archive | 2015

Treatment of Diseases and Conditions Caused by Increased Vascular Permeability

Larry R. Brown; Richard A. Banas; Howard Wessel; Elise M. Gill

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Brian C. Gilger

North Carolina State University

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Dana Fite

University of Pittsburgh

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David Culp

Research Triangle Park

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Kimberly Dine

University of Pennsylvania

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Reas S. Khan

University of Pennsylvania

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