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Brian C'K' Au, M'D'

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University of Texas Medical Branch Department of Ophthalmology ... Erythema. Chemosis. Discharge. Corneal Edema. Hypopyon. Cell Flare. Pressure 21 mmHg ... – PowerPoint PPT presentation

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Title: Brian C'K' Au, M'D'


1
  • Brian C.K. Au, M.D.
  • University of Arizona Department of
    Ophthalmology
  • University of Texas Medical Branch Department
    of Ophthalmology
  • ASCRS 2008 Annual Symposium Poster
  • April 5-9, 2008

2
Financial Disclosure
  • Brian C.K. Au, M.D. and co-authors do not have
    financial interests in any ophthalmic products or
    proprieties mentioned henceforth in this
    presentation.
  • Co-Authors (University of Arizona)
  • Jason W. Friday, M.S. IV
  • Stefano Lehman, M.D.
  • Robert W. Snyder, M.D., Ph.D.
  • Roxanna Ursea, M.D.

3
Introduction
  • Dislocation of the corneal donor button is a
    common post-operative complication and cause of
    decreased visual acuity in Descemets Stripping
    with Endothelial Keratoplasty (DSEK).
  • Clinical Question Is there a tool or substance
    that can
  • 1) Reduce the rate of donor button dislocation
    after DSEK?
  • 2) Effectively accomplish 1 without intraocular
    toxicity?

4
Purpose and Setting
  • Purpose
  • Part 1 To quantify the adhesive strength of
    Tisseel fibrin glue (Baxter, U.S.A.) when allowed
    to react in an in-vitro aqueous environment.
  • Part 2 To determine whether Tisseel is toxic
    when injected into the anterior chamber using a
    rabbit model.
  • Setting
  • Experimentation and Analysis University
    Laboratory, University of Arizona Department of
    Ophthalmology Tucson, Arizona, USA.
  • Creation of Virtual Poster University of Texas
    Medical Branch, Department of Ophthalmology and
    Visual Sciences Galveston, Texas, USA.

5
Methods Part 1 Adhesive Strength
  • The adhesive strength of Tisseel fibrin glue was
    tested by using a Penscale tension device (My
    Weigh, U.S.A.), which measures the amount of
    force required to displace a donor button from a
    native cornea. Five measurements were taken with
    no adhesive for control, then 10 measurements
    were taken following injection of Tisseel between
    the opposing corneal surfaces submerged in
    balanced salt solution (BSS).

6
Methods Part 2 Intracameral Toxicity
  • The toxicity of Tisseel was tested using five New
    Zealand white rabbits, where 0.05 mL of both the
    fibrin and thrombin components were injected into
    the anterior chamber. Rabbits were monitored and
    graded, on a scale of 0-10, for signs of toxicity
    post-operatively for seven days using a Panoptic
    ophthalmoscope and a Tono-pen.

7
Methods Tension Device
  • 10 donor 10 recipient New Zealand white rabbit
    clear corneas
  • Donor corneas (epithelium Descemets stripped)
    adhered to concave glass lens by superglue
  • Recipients corneas (epithelium Descemets
    stripped) adhered to convex epoxy lens by
    superglue
  • System submerged in BSS
  • Tisseel applied between donor and recipient
    corneal surfaces then surfaces apposed in-vitro
  • After 5 minutes, tension applied and weight
    required to separate corneal surfaces was recorded

8
Results
  • Part 1 Adhesive Strength The average force
    required to dislocate the donor button with no
    adhesive was found to be negligible at zero
    Newtons (N). The average force required to
    displace a donor button adhered with Tisseel was
    0.15N (plt0.003).
  • Part 2 Intracameral Toxicity The toxicity
    study showed only mild inflammation on
    post-operative day one (average grade of 1.8)
    which decreased to an average grade of 0.8 by day
    seven.

9
Results Part 1 Adhesive Strength
  • Table 1 Tension Device Readings. The initial
    weight of the glass lens with fixed recipient
    button, the weight at the moment of release, and
    the calculated difference yields the force of
    dislocation (F ma) against gravity (a
    9.8m/s2). Experimental groups were separated into
    those corneas previously submerged in BSS (Group
    1) and those that were used directly after
    preparation (Group 2).

10
Results Part 2 Intracameral Toxicity
  • Table 2. Rabbits were graded on 10 signs of
    inflammation using a Panoptic ophthalmoscope and
    a Tono-pen. Of note, rabbit 5 suffered a small
    puncture of the anterior capsule
    intraoperatively. While it was not removed from
    the experiment, this unintended trauma was taken
    into account when analyzing experimental results.

11
Results (4)
  • Rabbit 1 on post-operative day 7 graded as
    0/10.

12
Conclusion
  • Part 1 Adhesive Strength Tisseel fibrin
    adhesive reacts in an aqueous environment and
    provides ample force to prevent donor corneal
    button dislocation following DSEK in an in-vitro
    model.
  • Part 2 Intracameral Toxicity Tisseel appears
    to be non-toxic when injected into anterior
    chambers of rabbits. Intracameral use of Tisseel
    may reduce the rate of donor button dislocation
    following DSEK.
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