WO2010093772A1 - Method and apparatus for ocular surface imaging - Google Patents
Method and apparatus for ocular surface imaging Download PDFInfo
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- WO2010093772A1 WO2010093772A1 PCT/US2010/023865 US2010023865W WO2010093772A1 WO 2010093772 A1 WO2010093772 A1 WO 2010093772A1 US 2010023865 W US2010023865 W US 2010023865W WO 2010093772 A1 WO2010093772 A1 WO 2010093772A1
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61B—DIAGNOSIS; SURGERY; IDENTIFICATION
- A61B3/00—Apparatus for testing the eyes; Instruments for examining the eyes
- A61B3/10—Objective types, i.e. instruments for examining the eyes independent of the patients' perceptions or reactions
- A61B3/101—Objective types, i.e. instruments for examining the eyes independent of the patients' perceptions or reactions for examining the tear film
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61B—DIAGNOSIS; SURGERY; IDENTIFICATION
- A61B3/00—Apparatus for testing the eyes; Instruments for examining the eyes
- A61B3/10—Objective types, i.e. instruments for examining the eyes independent of the patients' perceptions or reactions
- A61B3/107—Objective types, i.e. instruments for examining the eyes independent of the patients' perceptions or reactions for determining the shape or measuring the curvature of the cornea
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61B—DIAGNOSIS; SURGERY; IDENTIFICATION
- A61B5/00—Measuring for diagnostic purposes; Identification of persons
- A61B5/0059—Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence
-
- G—PHYSICS
- G06—COMPUTING; CALCULATING OR COUNTING
- G06T—IMAGE DATA PROCESSING OR GENERATION, IN GENERAL
- G06T7/00—Image analysis
- G06T7/0002—Inspection of images, e.g. flaw detection
- G06T7/0012—Biomedical image inspection
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61B—DIAGNOSIS; SURGERY; IDENTIFICATION
- A61B3/00—Apparatus for testing the eyes; Instruments for examining the eyes
- A61B3/10—Objective types, i.e. instruments for examining the eyes independent of the patients' perceptions or reactions
- A61B3/14—Arrangements specially adapted for eye photography
-
- G—PHYSICS
- G06—COMPUTING; CALCULATING OR COUNTING
- G06T—IMAGE DATA PROCESSING OR GENERATION, IN GENERAL
- G06T2207/00—Indexing scheme for image analysis or image enhancement
- G06T2207/10—Image acquisition modality
- G06T2207/10004—Still image; Photographic image
- G06T2207/10012—Stereo images
-
- G—PHYSICS
- G06—COMPUTING; CALCULATING OR COUNTING
- G06T—IMAGE DATA PROCESSING OR GENERATION, IN GENERAL
- G06T2207/00—Indexing scheme for image analysis or image enhancement
- G06T2207/10—Image acquisition modality
- G06T2207/10056—Microscopic image
-
- G—PHYSICS
- G06—COMPUTING; CALCULATING OR COUNTING
- G06T—IMAGE DATA PROCESSING OR GENERATION, IN GENERAL
- G06T2207/00—Indexing scheme for image analysis or image enhancement
- G06T2207/10—Image acquisition modality
- G06T2207/10064—Fluorescence image
-
- G—PHYSICS
- G06—COMPUTING; CALCULATING OR COUNTING
- G06T—IMAGE DATA PROCESSING OR GENERATION, IN GENERAL
- G06T2207/00—Indexing scheme for image analysis or image enhancement
- G06T2207/30—Subject of image; Context of image processing
- G06T2207/30004—Biomedical image processing
- G06T2207/30041—Eye; Retina; Ophthalmic
Definitions
- the invention relates to apparatuses and methods for detecting corneal surface defects.
- An apparatus and method of the invention can be used to detect corneal surface diseases, such as dry eye.
- keratoconjunctivitis sicca dry eye
- One of the tests includes staining the ocular surface with a dye, followed by visual examination for stained surface defects. Lesions in the epithelial cell layers of the cornea adsorb stain and allow for the penetration of stain into interstitial spaces. The resultant bright speckled appearance of the otherwise black cornea is a hallmark pathology of cornea disease.
- Visual examination has been used since the early 1900s as a diagnostic for surface eye disease.
- the variability and reliability of these assessments has been poor when performed by individual physicians.
- quantitative image analysis of ocular surface images has proven difficult for at least three reasons.
- the first reason relates to Purkinje images of the illumination source in the images of the cornea and conjunctiva.
- the Purkinje image invariably interferes with image analysis and feature detection. Since it is not constant from one image to the next, such specular images are impossible to control for and must be removed prior to image analysis.
- Spectral methods are routinely used in fluorescence microscopy and whole body imaging to block undesired reflected light.
- Novitskaya et al. and Dean et al. described the use of a retinal camera having filtering properties for ocular surface stain imaging (Novitskaya et al., 2007, Contact Lens & Anterior Eye 30:258-259; Dean et al., 2008, Clinical and Experimental Ophthalmology 36:113-118).
- Novitskaya et al. and Dean et al. used digital fundus camera equipped with two filters, a blue exciter filter and a green bandpass filter, to detect fluorescence emitted from a fluorescein stained cornea.
- the fundus camera is designed to image fluorescein injected in to the vasculature as a means to assess retinal blood flow. The spectral properties of these filters were not described.
- a second difficulty in accurately detecting and measuring corneal stain relates to the methods used to capture corneal images. Any object in an image that is to be measured has to be in sharp focus in order to visually or mathematically delineate the boundaries of the object. Stained objects on the corneal surface reside on a highly curved surface and require the use of methods that increase the depth of focus or depth of field in the image.
- the average height of the cornea from the limbal edge to the apex, also called the sag height is 2.8 millimeters for the human eye.
- the standard of care diagnostic system for viewing and imaging the cornea uses a biomicroscope on a slit lamp that has a depth of field of 0.7 - 0.8 mm on average.
- any given stained corneal image from such a system can not possibly have all stained objects in sharp focus for subsequent analysis.
- Other imaging systems such as the retinal camera described by Novitskaya et al. and Dean et al. have a similar narrow depth of field for adequate image capture of the stained cornea.
- a third difficulty in accurately detecting and measuring corneal stain relates to the methods used to separate surface stained objects from surrounding image elements for subsequent measurement. Images of stained ocular surfaces from patients with dry eye or other ocular surface diseases generally have bright punctate stained objects of interest amidst a background fluorescence that is an unwanted signal and is not to be included in the measurement.
- the invention provides methods of detecting ocular surface diseases, the methods comprising: (a) illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is transmitted in a first predetermined wavelength range by an illumination filter positioned between the light source and the ocular surface, and wherein the light in the first predetermined wavelength range excites a contrast agent bound to defects on the ocular surface; and (b) detecting a light signal emitted from the contrast agent, wherein the light signal is transmitted in a second predetermined wavelength range by an imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device.
- the image capture device comprises an optical system with appropriate optics to increase depth of field in the image and transmits full field in focus image signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution.
- the invention further provides methods of detecting an ocular surface disease, the method comprising: (a) illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is polarized in a first orientation by an illumination filter positioned between the light source and the ocular surface, and wherein the light polarized in the first orientation excites a contrast agent bound to defects on the ocular surface; and (b) detecting a light signal emitted from the contrast agent, wherein the light signal is polarized in a second orientation by an imaging filter, and is transmitted by the imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device.
- the image capture device comprises an optical system with appropriate optics to increase depth of field in the image and transmits full field in focus image signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution in an automated fashion such that there is little or no human intervention in obtaining contrast agent distribution data.
- the contrast agent can be a fluorescent dye, a colored dye, or a natural substance, such as blood.
- the first filter and the second filter are polar filters, and are adjusted in opposite directions.
- the invention also provides an ocular surface examination apparatus, comprising: (a) a light source; (b) an illumination means for directing light along an illumination path onto an ocular surface; (c) an imaging means for directing reflected light from the ocular surface of a patient along an imaging path to enable an image of the ocular surface to be viewed; (d) an illumination filter that transmits light in the illumination path; and (e) an imaging filter that transmits reflected light in the imaging path, wherein the light in the illumination path can pass through the first filter, but cannot pass through the second filter.
- the invention also provides an ocular surface examination apparatus, comprising: (a) a light source for directing light along an illumination path onto an ocular surface; (b) an illumination filter that transmits light in the illumination path; (c) an imaging filter that transmits light reflected from a contrast agent on the ocular surface of a patient along an imaging path; and (d) an image capture device for detecting light reflected from the contrast agent on the ocular surface of the patient; wherein the light in the illumination path cannot pass through the imaging filter.
- FIG. 1 is a schematic diagram showing a configuration of an ophthalmic apparatus of the invention, wherein light in the illumination path 2 is reflected toward the ocular surface of an eye 9 via a half-mirror 4.
- FIG. 2 a schematic diagram showing a configuration of an ophthalmic apparatus of the invention, wherein light in the illumination path 2 is directed toward the ocular surface of an eye 9 via a ring light 4.
- FIG. 3 shows corneal images of a control patient (A) and a dry eye patient stained with 2% fluorescein solution for 3 min and imaged at 5 sec after blink.
- FIG. 4A shows an image of an artificial cornea obtained in ambient room light.
- FIG. 4B shows an image of an artificial cornea obtained with white excitation light and 532AF45 fluorescein emission filter.
- FIG. 4C shows an image of artificial cornea obtained with white excitation light and an HQ480/40 excitation filter in the illumination path.
- FIG. 5 A shows an image of a cornea stained with fluorescein.
- FIG. 5B shows an image of the fluorescein-stained cornea of FIG 5A after image processing with a Fourier bandpass filter
- FIG. 6A shows an image of a corneal surface collected using spectral filtering to capture distribution of fluorescein staining.
- FIG. 6B shows the image from FIG. 6A filtered with Fourier bandpass filters.
- FIG. 6C shows threshold segmentation of the image from FIG. 6B.
- FIG. 6D shows a measurement grid often referred the NEI (National Eye Institute) grid overlaid on to FIG. 6A.
- the NEI grid is most often used to manually score corneal staining by direct observation through a slit lamp of imaging device.
- FIG. 7 A shows an image of an ocular surface illuminated with left circularly polarized light.
- FIG. 7B shows an image of an ocular surface illuminated with left circular polarized light and imaged through a right circular polar filter.
- the invention relates to methods and apparatuses that can be used to quantitatively measure corneal staining.
- a method and apparatus of the invention can be used to capture images of a stained ocular surface (i.e. cornea) for the generation of objective information about ocular surface staining.
- the methods of the invention can be used, for example, as a diagnostic for ocular surface disease, such as dry eye, Sjogren's disease, infectious disease and contact lens wear problems, to measure therapeutic efficacy in clinical trials, or to measure efficacy of potential therapeutics in animal models of ocular surface diseases, such as dry eye.
- a method and/or apparatus of the invention comprises illuminating an ocular surface with a light that is filtered at a predetermined wavelength or polar orientation.
- the light travels along an illumination path toward the ocular surface, which comprises a contrast agent that can be excited by the light beam emitted from a light source.
- the light signal emitted from the contrast agent travels along an imaging path toward an image capture device, such as a camera.
- Cameras can be of several types including digital single lens reflex cameras with RGB CMOS sensors or black and white CCD cameras.
- the light signal captured by the image capture device is either spectrally isolated from the light in the illumination path, or has an opposite polar orientation relative to the light in the illumination path, as discussed in more detail below.
- a suitable contrast agent that can be used in a method and/or apparatus of the invention is any agent that can bind to a defect on the ocular surface and be detected by specific light absorption and emission characteristics (i.e. color or fluorescence emission).
- fluorescein, lissamine green, rose bengal have been used to measure surface irritation associated with dry eye (Bron et al, 2003, Cornea 22:640- 650) and contact lens wear (Begley et al, 1994, Int Contact Lens Clin 21:7-13.).
- a contrast agent can be administered to a patient via an eye drop, for example, aqueous solutions of sodium fluorescein or lissamine green are typically instilled as a one to five microliter drop onto the surface of the eye.
- a contrast agent can be administered from a dye impregnated strip, such as sodium fluorescein impregnated strip (FluoretsTM; Chauvin Pharmaceuticals, Essex, United Kingdom), in which a wetted strip is placed in contact with the eye at the lower lid margin for a period of a few minutes.
- a "patient” can be any mammal.
- the patient is a human, monkey, rabbit, mouse, or rat. Most preferably, the patient is a human.
- FIG. 1 provides a schematic diagram showing one configuration of an ophthalmic apparatus of the invention.
- a light source 1 emits light in an illumination path 2 toward a half-mirror 4.
- the light in the illumination path 2 passes through an illumination filter 3, then contacts the half-mirror 4, and is reflected toward the surface of an eye 9.
- the light in the illumination path 2 is adapted to excite a contrast agent present on the surface of the eye.
- a light signal emitted from the excited contrast agent travels in an imaging path 8 toward a lens 5.
- An imaging filter 7 is positioned in the imaging path 8 between the ocular surface of the eye 9 and the lens 5.
- Images of corneal surface defects are captured by an image capture device 6 and transmitted to a machine readable storage medium 10.
- the machine readable storage medium 10 comprises instructions for providing quantitative analysis of contrast agent intensity and distribution. Images of corneal surface defects can be visualized via a display unit, such as a monitor, that is connected to the machine readable storage medium 10.
- FIG. 2 shows a schematic diagram showing another configuration of an ophthalmic apparatus of the invention.
- a light source 1 emits light in an illumination path 2 toward an illumination device 4.
- the illumination device can be, for example, a fiber optic ring light.
- the light in the illumination path 2 passes through an illumination filter 3, then contacts the illumination device 4, which transmits the light toward the surface of an eye 9.
- the light in the illumination path 2 is adapted to excite a contrast agent present on the surface of the eye.
- Light emitted from the excited contrast agent travels in an imaging path 8 toward a lens 5.
- An imaging filter 7 is positioned in the imaging path 8 between the ocular surface of the eye 9 and the lens 5.
- Images of corneal surface defects are captured by an image capture device 6 and transmitted to a machine readable storage medium 10.
- the machine readable storage medium 10 comprises instructions for providing quantitative analysis of contrast agent intensity and distribution. Images of corneal surface defects can be visualized via a display unit, such as a monitor, that is connected to the machine readable storage medium 10.
- illumination of the ocular surface using a method and/or apparatus of the invention is accomplished with light having specific wavelength ranges and/or polarized light, and images of the ocular surface are captured at specific wavelength ranges and/or polarization to produce images that are free of specular images of the illumination system.
- the wavelength range of light used to illuminate the ocular surface is spectrally isolated from the light used to capture the images (i.e. the light in the illumination path 2 cannot pass through the filter 7 in the imaging path 8).
- Spectral isolation of the light in an illumination path 2 from that in the imaging path 8 can be accomplished, for example, using a set of bandpass filters, one filter for illumination and a different filter for image capture.
- a method and/or apparatus of the invention can comprise an illumination filter 3 that can transmit light in a range of 465 - 500 nanometers, for optimum excitation of fluorescein, and an imaging filter 7 that can transmit light greater than 515 nanometers, for optimum detection of fluorescein.
- an illumination filter 3 that can transmit light in a range of 465 - 500 nanometers, for optimum excitation of fluorescein
- an imaging filter 7 that can transmit light greater than 515 nanometers, for optimum detection of fluorescein.
- other wavelength ranges for absorption and detection would be preferred.
- the optical density for each filter outside of these ranges would be at least 5.0 (i.e., transmittance greater than or equal to 0.000001).
- a method and/or apparatus of the invention comprises polarized light to illuminate the ocular surface, wherein the illumination filter 3 and the imaging filter 7 are polar filters.
- the ocular surface of an eye is illuminated with circularly polarized light, using an illumination filter 3 that is a left or right circular polar filter, and the imaging filter 7 is a right or left circular polar filter, respectively (i.e. where the illumination filter 3 is a left circular polar filter, the imaging filter 7 is a right circular polar filter).
- the ocular surface of an eye is illuminated with plane polarized light, wherein the illumination filter 3 and imaging filter 7 are adjusted in opposite directions.
- the arrangement (i.e. the illumination filter and the imaging filter are in different light paths) and properties of the filters in an apparatus and/or method of the invention ensures that an accurate image of ocular surface defects is captured, wherein the image is free from illumination artifacts (e.g. specular or Purkinje images from the light source).
- the contrast agent is a fluorescent dye
- the illumination filter can be selected to transmit light in a particular range of wavelengths capable of exciting the dye
- the imaging filter can be selected to transmit light at wavelengths that are outside the wavebands transmitted by the illumination filter.
- the imaging filter will transmit fluorescence from the dye while blocking fluorescence that is generated from other objects on the ocular surface.
- images of corneal surface defects are captured by an image capture device, where they are stored and/or transferred to a machine readable storage medium.
- the machine readable storage medium comprises a program of instructions stored thereon for causing an electrical processor to execute automated method steps for image analysis, which is performed using an adaptive threshold algorithm, in conjunction with the light filtering accomplished with the illumination filter and the imaging filter, to segment stained objects from digital images.
- the adaptive threshold method iteratively adjusts the segmentation threshold until the rate of change in the number of pixels in the segmented image has reached a predetermined level.
- an optical system can be used to increase depth of field in an image captured using a method or apparatus of the invention.
- an "optical system” can be used to place an aperture in the optical imaging path that increases the depth of focus in the final image, or to adjust the focal plane of the imaging system such that several images collected at different focal planes are collected and electronically rendered into a single in- focus image of the ocular surface (e.g. extended depth of field rendering).
- the optical system can be incorporated into an image capture device. An image that has been adjusted using the optical system is transmitted as a full field, in-focus image to a machine readable storage medium that comprises instructions that provide automated, quantitative analysis of contrast agent intensity and distribution. Automated analysis eliminates the possibility of human error in obtaining and/or interpreting the contrast agent distribution data.
- a method and/or apparatus of the invention can comprise the use of Fourier bandpass filtering to enhance and aid subsequent stained object detection.
- Fourier image processing is based on the work of the French mathematician
- the Fourier transform is the mathematical operation that transforms the original measure or signal into an expression of complex exponentials with a range of amplitude coefficients and frequency terms.
- An image being a two dimensional array of intensity measurements, can also be transformed to two dimensional arrays of complex exponentials. This Fourier transformation is often referred to as a transformation from the spatial domain to the frequency domain. In the frequency domain, one can highlight specific structures and remove others for subsequent analysis by removing certain frequencies from the transform and then calculating the inverse transform.
- the bright conjunctiva surrounding the cornea and the diffuse background fluorescence are represented by lower frequency terms in the transform while stained spots are represented by high frequency terms.
- a Fourier band pass filter can be used with a predetermined frequency space to remove low frequency components
- Example 1 Spectral filtering removes Purkinje images of the illumination source from images of specular surfaces
- the ability to spectrally remove the specular or Purkinje image from ocular surface fluorescence images was demonstrated with an artificial cornea prepared from a hard contact lens.
- a hard contact lens made of polymethylmethacrylate was coated with green fluorescent beads, (Bangs Laboratories, Inc, Fishers, IN) to simulate stained spots on a curve corneal surface. The spectral properties of these beads were similar to fluorescein.
- the artificial cornea was position in front of a Nikon digital single lens reflex camera and illuminated with a fiber optic ring light mounted to the lens of the camera.
- the fiber optic ring illuminator was configured such that band pass filters could be used to spectrally define the light emanating from the ring. Images were collected through either a green bandpass filter optimized for fluorescein emission wavelengths, (532 +/- 45 nm) or no filter.
- the artificial cornea coated with fluorescent beads is shown in FIG. 3A illuminated with ambient white room light and imaged without a green blocking filter. A specular image of the dim room lamp was observed on the upper side of the lens surface.
- the artificial cornea was illuminated with white light from a fiber optic ring light and an image was collected through the green bandpass filter. A bright specular image of the ring light was observed.
- the artificial cornea was illuminated with filtered blue light, 480 +/- 40 nm; though the ring light and the images were collected with the green bandpass filter. The specular image of the ring was no longer observed and the fluorescent beads coating the surface became observable.
- the use of two filters, one for excitation and one for image collection, having non-overlapping wavelength ranges eliminated the specular image of the source illumination and allowed the beads to be more easily and consistently measured.
- Spectral filtering removes Purkinje images of the illumination source from images of the ocular surface
- a severe dry eye patient and a non-dry eye patient were subjected to corneal staining with 5 ⁇ L of 2% sodium fluorescein for 3 minutes, followed by a saline wash
- the stained eyes were imaged with a Haag-Streit BX-900 slit lamp.
- the Haag-Streit slit lamp consisted of a stereo biomicroscope, a combination flash lamp and modeling lamp for illuminating the eye and a Canon 4OD digital camera and computer for image capture.
- the slit lamp was modified by the addition of a fluorescein excitation bandpass filter to the flash lamp output and the insertion of a fluorescein emission filter in the light path to the between the eye and the camera.
- the fluorescein excitation filter had a bandpass (transmission > 90%) of 483 +/- 32 nm and the emission filter had a bandpass of 536 +/- 40 nm.
- the out-of-band optical densities of these custom filters was designed to be > 6, hence no excitation light passed into the camera.
- corneal images from the control non-dry eye subject (A) revealed a relatively uniform cornea with no obvious stained lesions, while from the dry eye subject (B) exhibited with several brightly stained punctate spotss.
- the spots represented defects or lesions in the corneal epithelial layer associated with the dry eye condition.
- FIG. 5 and FIG. 6 The effect of the Fourier bandpass filtering process was illustrated in FIG. 5 and FIG. 6.
- the fluorescein corneal image in FIG. 5A was obtained with a camera based imaging system equipped with fluorescein spectral band pass filters as described above.
- the two dimensional Fourier transform of the image in FIG 5 A was then calculated using an unpadded fast Fourier transform algorithm found in most image analysis software.
- the transform was then multiplied by the Fourier transform of a low pass Gaussian filter and the inverse transform of the product was calculated to produce the image in FIG 5B.
- the Fourier processing removed the low background brightness of the conjunctiva and background stain leading to an enhancement of the small speckled stained structures in the cornea (compare image in FIG.5A and FIG.5B).
- FIG. 6A-D The utility of the imaging method and the Fourier bandpass filtering process in measuring fluorescein stained objected in corneas is illustrated in FIG. 6A-D.
- FIG. 8A the image collected using spectral filtering method captured the distribution of fluorescein staining on human cornea without Purkinje image of the lamp.
- the image in FIG. 6A was filtered using Fourier bandpass, to highlight fluorescein stained objects (FIG. 6B). Threshold segmentation of the image in FIG. 6B was performed, such that group pixels above a certain threshold intensity and size were isolated and overlaid in green.
- FIG. 8A the image collected using spectral filtering method captured the distribution of fluorescein staining on human cornea without Purkinje image of the lamp.
- the image in FIG. 6A was filtered using Fourier bandpass, to highlight fluorescein stained objects (FIG. 6B). Threshold segmentation of the image in FIG. 6B was performed, such that group pixels above a certain threshold intensity and
- 6D shows detected objects illustrated in 6C along with a standard corneal scoring grid commonly referred to as the National Eye Institute (NEI) grid, recommended by the National Eye Institute for visually scoring staining use, (Lemp MA. Report of the National Eye Institute/Industry workshop on Clinical Trials in Dry Eyes CLAO J. 1995 Oct;21(4):221-32).
- NAI National Eye Institute
- the need to remove specular images of the illumination source from ocular surface images is not limited to fluorescein stained eyes.
- ocular examinations such as measuring hyperemia or colored conjunctival stains, such as lissamine green or rose bengal, it would be advantageous to remove the specular images of the source to facilitate subsequent analysis.
- polarization optics can be used to filter specular reflected light from ocular images. An example of this is shown in FIG. 7
- FIG. 7A shows an image of an ocular surface obtained by illuminating with left circularly polarized light using a ring light source and imaged without a polar filter in the eye to camera light path.
- the specular image of the ring light appeared as a bright white ring in the center of the eye (FIG. 7A).
- FIG. 7B shows an image of the ocular surface illuminated with left circular polarized light using the same ring light source and imaged through a right circular polar filter in the eye to camera light path.
- the specular reflected light from the ring light was blocked by the cross polar filter and the image was free of specular artifact (FIG. 7B).
- polarized light filtering eliminated the Purkinje artifacts from the ocular surface image.
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Abstract
The invention provides apparatuses and methods for detecting corneal surface defects. The methods and/or an apparatus of the invention can be used to detect corneal surface diseases, such as dry eye.
Description
METHOD AND APPARATUS FOR OCULAR SURFACE IMAGING
CROSS-REFERENCE TO RELATED APPLICATION
This application claims priority under 35 U. S. C. §119 to U.S. Provisional Patent Application No. 61/151,880 filed February 12, 2009, the entire contents of which are incorporated herein by reference.
FIELD OF THE INVENTION
The invention relates to apparatuses and methods for detecting corneal surface defects. An apparatus and method of the invention can be used to detect corneal surface diseases, such as dry eye.
BACKGROUND OF THE INVENTION
The diagnosis and prognosis of ocular surface diseases, such as keratoconjunctivitis sicca (dry eye), involves several tests. One of the tests includes staining the ocular surface with a dye, followed by visual examination for stained surface defects. Lesions in the epithelial cell layers of the cornea adsorb stain and allow for the penetration of stain into interstitial spaces. The resultant bright speckled appearance of the otherwise black cornea is a hallmark pathology of cornea disease. Visual examination has been used since the early 1900s as a diagnostic for surface eye disease. However, the variability and reliability of these assessments has been poor when performed by individual physicians. Hence there is an urgent need for a consistent measure of surface staining that is free of human bias and error. Heretofore, quantitative image analysis of ocular surface images has proven difficult for at least three reasons.
The first reason relates to Purkinje images of the illumination source in the images of the cornea and conjunctiva. The Purkinje image invariably interferes with image analysis and feature detection. Since it is not constant from one image to the next, such specular images are impossible to control for and must be removed prior to image analysis. Spectral methods are routinely used in fluorescence microscopy and whole body imaging to block undesired reflected light. Novitskaya et al. and Dean et
al. described the use of a retinal camera having filtering properties for ocular surface stain imaging (Novitskaya et al., 2007, Contact Lens & Anterior Eye 30:258-259; Dean et al., 2008, Clinical and Experimental Ophthalmology 36:113-118). Novitskaya et al. and Dean et al. used digital fundus camera equipped with two filters, a blue exciter filter and a green bandpass filter, to detect fluorescence emitted from a fluorescein stained cornea. The fundus camera is designed to image fluorescein injected in to the vasculature as a means to assess retinal blood flow. The spectral properties of these filters were not described.
A second difficulty in accurately detecting and measuring corneal stain relates to the methods used to capture corneal images. Any object in an image that is to be measured has to be in sharp focus in order to visually or mathematically delineate the boundaries of the object. Stained objects on the corneal surface reside on a highly curved surface and require the use of methods that increase the depth of focus or depth of field in the image. The average height of the cornea from the limbal edge to the apex, also called the sag height is 2.8 millimeters for the human eye. The standard of care diagnostic system for viewing and imaging the cornea uses a biomicroscope on a slit lamp that has a depth of field of 0.7 - 0.8 mm on average. Hence any given stained corneal image from such a system can not possibly have all stained objects in sharp focus for subsequent analysis. Other imaging systems such as the retinal camera described by Novitskaya et al. and Dean et al. have a similar narrow depth of field for adequate image capture of the stained cornea.
A third difficulty in accurately detecting and measuring corneal stain relates to the methods used to separate surface stained objects from surrounding image elements for subsequent measurement. Images of stained ocular surfaces from patients with dry eye or other ocular surface diseases generally have bright punctate stained objects of interest amidst a background fluorescence that is an unwanted signal and is not to be included in the measurement.
Consequently, there is a need in the art to eliminate unwanted specular images in corneal staining and to capture full field in focus images of the corneal surface while enhancing a light signal that represents ocular surface defects for accurate diagnosis and monitoring of corneal surface diseases.
SUMMARY OF THE INVENTION
The invention provides methods of detecting ocular surface diseases, the methods comprising: (a) illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is transmitted in a first predetermined wavelength range by an illumination filter positioned between the light source and the ocular surface, and wherein the light in the first predetermined wavelength range excites a contrast agent bound to defects on the ocular surface; and (b) detecting a light signal emitted from the contrast agent, wherein the light signal is transmitted in a second predetermined wavelength range by an imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device. In one aspect, the image capture device comprises an optical system with appropriate optics to increase depth of field in the image and transmits full field in focus image signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution.
The invention further provides methods of detecting an ocular surface disease, the method comprising: (a) illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is polarized in a first orientation by an illumination filter positioned between the light source and the ocular surface, and wherein the light polarized in the first orientation excites a contrast agent bound to defects on the ocular surface; and (b) detecting a light signal emitted from the contrast agent, wherein the light signal is polarized in a second orientation by an imaging filter, and is transmitted by the imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device. In one aspect, the image capture device comprises an optical system with appropriate optics to increase depth of field in the image and transmits full field in focus image signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution in an automated fashion such that there is little or no human intervention in obtaining contrast agent distribution data.
In certain aspects, the contrast agent can be a fluorescent dye, a colored dye, or a natural substance, such as blood.
In yet another aspect, the first filter and the second filter are polar filters, and are adjusted in opposite directions.
The invention also provides an ocular surface examination apparatus, comprising: (a) a light source; (b) an illumination means for directing light along an illumination path onto an ocular surface; (c) an imaging means for directing reflected light from the ocular surface of a patient along an imaging path to enable an image of the ocular surface to be viewed; (d) an illumination filter that transmits light in the illumination path; and (e) an imaging filter that transmits reflected light in the imaging path, wherein the light in the illumination path can pass through the first filter, but cannot pass through the second filter.
The invention also provides an ocular surface examination apparatus, comprising: (a) a light source for directing light along an illumination path onto an ocular surface; (b) an illumination filter that transmits light in the illumination path; (c) an imaging filter that transmits light reflected from a contrast agent on the ocular surface of a patient along an imaging path; and (d) an image capture device for detecting light reflected from the contrast agent on the ocular surface of the patient; wherein the light in the illumination path cannot pass through the imaging filter.
Specific preferred embodiments of the invention will become evident from the following more detailed description of certain preferred embodiments and the claims.
BRIEF DESCRIPTION OF THE DRAWINGS
FIG. 1 is a schematic diagram showing a configuration of an ophthalmic apparatus of the invention, wherein light in the illumination path 2 is reflected toward the ocular surface of an eye 9 via a half-mirror 4. FIG. 2 a schematic diagram showing a configuration of an ophthalmic apparatus of the invention, wherein light in the illumination path 2 is directed toward the ocular surface of an eye 9 via a ring light 4.
FIG. 3 shows corneal images of a control patient (A) and a dry eye patient stained with 2% fluorescein solution for 3 min and imaged at 5 sec after blink. FIG. 4A shows an image of an artificial cornea obtained in ambient room light.
FIG. 4B shows an image of an artificial cornea obtained with white excitation light and 532AF45 fluorescein emission filter.
FIG. 4C shows an image of artificial cornea obtained with white excitation light and an HQ480/40 excitation filter in the illumination path. FIG. 5 A shows an image of a cornea stained with fluorescein.
FIG. 5B shows an image of the fluorescein-stained cornea of FIG 5A after image processing with a Fourier bandpass filter
FIG. 6A shows an image of a corneal surface collected using spectral filtering to capture distribution of fluorescein staining. FIG. 6B shows the image from FIG. 6A filtered with Fourier bandpass filters.
FIG. 6C shows threshold segmentation of the image from FIG. 6B.
FIG. 6D shows a measurement grid often referred the NEI (National Eye Institute) grid overlaid on to FIG. 6A. The NEI grid is most often used to manually score corneal staining by direct observation through a slit lamp of imaging device. FIG. 7 A shows an image of an ocular surface illuminated with left circularly polarized light.
FIG. 7B shows an image of an ocular surface illuminated with left circular polarized light and imaged through a right circular polar filter.
DETAILED DESCRIPTION
The invention relates to methods and apparatuses that can be used to quantitatively measure corneal staining. In particular, a method and apparatus of the invention can be used to capture images of a stained ocular surface (i.e. cornea) for the generation of objective information about ocular surface staining. The methods of the invention can be used, for example, as a diagnostic for ocular surface disease, such as dry eye, Sjogren's disease, infectious disease and contact lens wear problems, to measure therapeutic efficacy in clinical trials, or to measure efficacy of potential therapeutics in animal models of ocular surface diseases, such as dry eye.
Exemplary configurations of an apparatus of the invention are shown in FIG. 1 and FIG. 2, and are discussed in detail below.
In certain embodiments, a method and/or apparatus of the invention comprises illuminating an ocular surface with a light that is filtered at a predetermined wavelength or polar orientation. The light travels along an illumination path toward the ocular surface, which comprises a contrast agent that can be excited by the light beam emitted from a light source. The light signal emitted from the contrast agent travels along an imaging path toward an image capture device, such as a camera. Cameras can be of several types including digital single lens reflex cameras with RGB CMOS sensors or black and white CCD cameras. In a particular embodiment, the light signal captured by the image capture device is either spectrally isolated from the light in the illumination path, or has an opposite polar orientation relative to the light in the illumination path, as discussed in more detail below.
A suitable contrast agent that can be used in a method and/or apparatus of the invention is any agent that can bind to a defect on the ocular surface and be detected by specific light absorption and emission characteristics (i.e. color or fluorescence emission). For example, fluorescein, lissamine green, rose bengal have been used to measure surface irritation associated with dry eye (Bron et al, 2003, Cornea 22:640- 650) and contact lens wear (Begley et al, 1994, Int Contact Lens Clin 21:7-13.). A contrast agent can be administered to a patient via an eye drop, for example, aqueous solutions of sodium fluorescein or lissamine green are typically instilled as a one to five microliter drop onto the surface of the eye.
Alternatively, a contrast agent can be administered from a dye impregnated strip, such as sodium fluorescein impregnated strip (Fluorets™; Chauvin Pharmaceuticals, Essex, United Kingdom), in which a wetted strip is placed in contact with the eye at the lower lid margin for a period of a few minutes. As used herein, a "patient" can be any mammal. Preferably, the patient is a human, monkey, rabbit, mouse, or rat. Most preferably, the patient is a human.
FIG. 1 provides a schematic diagram showing one configuration of an ophthalmic apparatus of the invention.
Referring to FIG. 1, a light source 1 emits light in an illumination path 2 toward a half-mirror 4. The light in the illumination path 2 passes through an illumination filter 3, then contacts the half-mirror 4, and is reflected toward the surface of an eye 9. The light in the illumination path 2 is adapted to excite a contrast
agent present on the surface of the eye. A light signal emitted from the excited contrast agent travels in an imaging path 8 toward a lens 5. An imaging filter 7 is positioned in the imaging path 8 between the ocular surface of the eye 9 and the lens 5. Images of corneal surface defects are captured by an image capture device 6 and transmitted to a machine readable storage medium 10. The machine readable storage medium 10 comprises instructions for providing quantitative analysis of contrast agent intensity and distribution. Images of corneal surface defects can be visualized via a display unit, such as a monitor, that is connected to the machine readable storage medium 10.
FIG. 2 shows a schematic diagram showing another configuration of an ophthalmic apparatus of the invention.
Referring to FIG. 2, a light source 1 emits light in an illumination path 2 toward an illumination device 4. The illumination device can be, for example, a fiber optic ring light. The light in the illumination path 2 passes through an illumination filter 3, then contacts the illumination device 4, which transmits the light toward the surface of an eye 9. The light in the illumination path 2 is adapted to excite a contrast agent present on the surface of the eye. Light emitted from the excited contrast agent travels in an imaging path 8 toward a lens 5. An imaging filter 7 is positioned in the imaging path 8 between the ocular surface of the eye 9 and the lens 5.
Images of corneal surface defects are captured by an image capture device 6 and transmitted to a machine readable storage medium 10. The machine readable storage medium 10 comprises instructions for providing quantitative analysis of contrast agent intensity and distribution. Images of corneal surface defects can be visualized via a display unit, such as a monitor, that is connected to the machine readable storage medium 10.
In certain embodiments, illumination of the ocular surface using a method and/or apparatus of the invention is accomplished with light having specific wavelength ranges and/or polarized light, and images of the ocular surface are captured at specific wavelength ranges and/or polarization to produce images that are free of specular images of the illumination system.
In one embodiment, the wavelength range of light used to illuminate the ocular surface is spectrally isolated from the light used to capture the images (i.e. the light in the illumination path 2 cannot pass through the filter 7 in the imaging path 8). Spectral isolation of the light in an illumination path 2 from that in the imaging path 8 can be accomplished, for example, using a set of bandpass filters, one filter for illumination and a different filter for image capture. The wavelength range of the two filters cannot overlap, and therefore have very large out-of-band optical densities. Consequently, no light from the light source 1 can pass into the image capture device 6 and be imaged. For example, where fluorescein is a contrast agent on the ocular surface of the eye 9, a method and/or apparatus of the invention can comprise an illumination filter 3 that can transmit light in a range of 465 - 500 nanometers, for optimum excitation of fluorescein, and an imaging filter 7 that can transmit light greater than 515 nanometers, for optimum detection of fluorescein. Depending on the spectral properties of the contrast agent, other wavelength ranges for absorption and detection would be preferred. The optical density for each filter outside of these ranges would be at least 5.0 (i.e., transmittance greater than or equal to 0.000001).
In another embodiment, a method and/or apparatus of the invention comprises polarized light to illuminate the ocular surface, wherein the illumination filter 3 and the imaging filter 7 are polar filters. For example, the ocular surface of an eye is illuminated with circularly polarized light, using an illumination filter 3 that is a left or right circular polar filter, and the imaging filter 7 is a right or left circular polar filter, respectively (i.e. where the illumination filter 3 is a left circular polar filter, the imaging filter 7 is a right circular polar filter). Alternatively, the ocular surface of an eye is illuminated with plane polarized light, wherein the illumination filter 3 and imaging filter 7 are adjusted in opposite directions.
The arrangement (i.e. the illumination filter and the imaging filter are in different light paths) and properties of the filters in an apparatus and/or method of the invention ensures that an accurate image of ocular surface defects is captured, wherein the image is free from illumination artifacts (e.g. specular or Purkinje images from the light source). For example, where the contrast agent is a fluorescent dye, the illumination filter can be selected to transmit light in a particular range of wavelengths capable of exciting the dye, while the imaging filter can be selected to transmit light at wavelengths that are outside the wavebands transmitted by the
illumination filter. The imaging filter will transmit fluorescence from the dye while blocking fluorescence that is generated from other objects on the ocular surface. Thus, the only signal captured for analysis will be associated with defects on the ocular surface that are bound to the dye. In certain embodiments, images of corneal surface defects are captured by an image capture device, where they are stored and/or transferred to a machine readable storage medium. The machine readable storage medium comprises a program of instructions stored thereon for causing an electrical processor to execute automated method steps for image analysis, which is performed using an adaptive threshold algorithm, in conjunction with the light filtering accomplished with the illumination filter and the imaging filter, to segment stained objects from digital images. The adaptive threshold method iteratively adjusts the segmentation threshold until the rate of change in the number of pixels in the segmented image has reached a predetermined level. In other embodiments, an optical system can be used to increase depth of field in an image captured using a method or apparatus of the invention. For example, an "optical system" can be used to place an aperture in the optical imaging path that increases the depth of focus in the final image, or to adjust the focal plane of the imaging system such that several images collected at different focal planes are collected and electronically rendered into a single in- focus image of the ocular surface (e.g. extended depth of field rendering). In certain embodiments, the optical system can be incorporated into an image capture device. An image that has been adjusted using the optical system is transmitted as a full field, in-focus image to a machine readable storage medium that comprises instructions that provide automated, quantitative analysis of contrast agent intensity and distribution. Automated analysis eliminates the possibility of human error in obtaining and/or interpreting the contrast agent distribution data.
The isolation or segmentation of stained objects in corneas stained with a contrast agent for size position and intensity measurements is not obvious, despite the fact the stained objects can be more quickly visualized in properly filtered, in-focus images. Faint background fluorescence of residual stain in the tear film and autofluorescence from the cornea and surrounding conjunctiva require the use of image processing to highlight the stained spots. Fourier image processing methods
are one of several means to enhance the appearance and subsequent threshold segmentation of image objects. In certain embodiments, a method and/or apparatus of the invention can comprise the use of Fourier bandpass filtering to enhance and aid subsequent stained object detection. Fourier image processing is based on the work of the French mathematician
Jean Baptiste Joseph Fourier, which postulates that any measurement in time and space can be expressed as an equation of sin and cosine functions or, to use the Euler formula, a series of complex exponentials summed over an infinite range of frequencies. The Fourier transform is the mathematical operation that transforms the original measure or signal into an expression of complex exponentials with a range of amplitude coefficients and frequency terms. An image, being a two dimensional array of intensity measurements, can also be transformed to two dimensional arrays of complex exponentials. This Fourier transformation is often referred to as a transformation from the spatial domain to the frequency domain. In the frequency domain, one can highlight specific structures and remove others for subsequent analysis by removing certain frequencies from the transform and then calculating the inverse transform. For example, in stained cornea images, the bright conjunctiva surrounding the cornea and the diffuse background fluorescence are represented by lower frequency terms in the transform while stained spots are represented by high frequency terms. By multiplying the transform of the original image with a filter that reduces the low frequency terms and performing an inverse transform on the product, an image is created that has reduced the diffuse background and conjunctival intensities while maintaining the stained spots.
Thus, in certain embodiments of the invention, a Fourier band pass filter can be used with a predetermined frequency space to remove low frequency components
(i.e., very large objects or background) and highlight high frequency components that include small punctate objects. Examples of potential filters include, but are not limited to, Gaussian and Butterworth filters. Fourier filtering advantageously permits detection of punctate stained regions against a varying background of unbound stain in the tear film (see Example 2 below, which illustrates process and results of Fourier band pass filter for detecting stained objects on the ocular surface).
All references cited in this application are expressly incorporated by reference herein for any purpose.
Unless otherwise required by context, singular terms used herein shall include pluralities and plural terms shall include the singular.
EXAMPLES The following examples, including the experiments conducted and results achieved are provided for illustrative purposes only and are not to be construed as limiting the invention.
Example 1 Spectral filtering removes Purkinje images of the illumination source from images of specular surfaces
The ability to spectrally remove the specular or Purkinje image from ocular surface fluorescence images was demonstrated with an artificial cornea prepared from a hard contact lens. For this a hard contact lens made of polymethylmethacrylate was coated with green fluorescent beads, (Bangs Laboratories, Inc, Fishers, IN) to simulate stained spots on a curve corneal surface. The spectral properties of these beads were similar to fluorescein. The artificial cornea was position in front of a Nikon digital single lens reflex camera and illuminated with a fiber optic ring light mounted to the lens of the camera. The fiber optic ring illuminator was configured such that band pass filters could be used to spectrally define the light emanating from the ring. Images were collected through either a green bandpass filter optimized for fluorescein emission wavelengths, (532 +/- 45 nm) or no filter.
The artificial cornea coated with fluorescent beads is shown in FIG. 3A illuminated with ambient white room light and imaged without a green blocking filter. A specular image of the dim room lamp was observed on the upper side of the lens surface. In Figure 3B, the artificial cornea was illuminated with white light from a fiber optic ring light and an image was collected through the green bandpass filter. A bright specular image of the ring light was observed. In Figure 3C, the artificial cornea was illuminated with filtered blue light, 480 +/- 40 nm; though the ring light and the images were collected with the green bandpass filter. The specular image of the ring was no longer observed and the fluorescent beads coating the surface became
observable. The use of two filters, one for excitation and one for image collection, having non-overlapping wavelength ranges eliminated the specular image of the source illumination and allowed the beads to be more easily and consistently measured.
Example 2
Spectral filtering removes Purkinje images of the illumination source from images of the ocular surface
A severe dry eye patient and a non-dry eye patient were subjected to corneal staining with 5 μL of 2% sodium fluorescein for 3 minutes, followed by a saline wash
(Unisol 4 Saline Solution, Alcon Laboratories, Inc., Fort Worth, TX). The stained eyes were imaged with a Haag-Streit BX-900 slit lamp. The Haag-Streit slit lamp consisted of a stereo biomicroscope, a combination flash lamp and modeling lamp for illuminating the eye and a Canon 4OD digital camera and computer for image capture. The slit lamp was modified by the addition of a fluorescein excitation bandpass filter to the flash lamp output and the insertion of a fluorescein emission filter in the light path to the between the eye and the camera. The fluorescein excitation filter had a bandpass (transmission > 90%) of 483 +/- 32 nm and the emission filter had a bandpass of 536 +/- 40 nm. The out-of-band optical densities of these custom filters was designed to be > 6, hence no excitation light passed into the camera.
As shown in FIG. 4, corneal images from the control non-dry eye subject (A) revealed a relatively uniform cornea with no obvious stained lesions, while from the dry eye subject (B) exhibited with several brightly stained punctate spotss. The spots represented defects or lesions in the corneal epithelial layer associated with the dry eye condition. These images were suitable for quantifying the position, size, intensity and shape of the stained lesions. Again there were no Purkinje images of the illuminating source in these images.
Example 3 Fourier Analysis of Ocular Surface Defects of a Dry Eye Patient
The effect of the Fourier bandpass filtering process was illustrated in FIG. 5 and FIG. 6. The fluorescein corneal image in FIG. 5A was obtained with a camera based imaging system equipped with fluorescein spectral band pass filters as described above. The two dimensional Fourier transform of the image in FIG 5 A was then calculated using an unpadded fast Fourier transform algorithm found in most image analysis software. The transform was then multiplied by the Fourier transform of a low pass Gaussian filter and the inverse transform of the product was calculated to produce the image in FIG 5B. As expected, the Fourier processing removed the low background brightness of the conjunctiva and background stain leading to an enhancement of the small speckled stained structures in the cornea (compare image in FIG.5A and FIG.5B). The utility of the imaging method and the Fourier bandpass filtering process in measuring fluorescein stained objected in corneas is illustrated in FIG. 6A-D. As shown in FIG. 8A, the image collected using spectral filtering method captured the distribution of fluorescein staining on human cornea without Purkinje image of the lamp. The image in FIG. 6A was filtered using Fourier bandpass, to highlight fluorescein stained objects (FIG. 6B). Threshold segmentation of the image in FIG. 6B was performed, such that group pixels above a certain threshold intensity and size were isolated and overlaid in green. FIG. 6D shows detected objects illustrated in 6C along with a standard corneal scoring grid commonly referred to as the National Eye Institute (NEI) grid, recommended by the National Eye Institute for visually scoring staining use, (Lemp MA. Report of the National Eye Institute/Industry workshop on Clinical Trials in Dry Eyes CLAO J. 1995 Oct;21(4):221-32). These results demonstrated that Fourier processing allowed one to enhance contrast in an image based on the size of object, and was independent of the objects mean intensity when compared to threshold based methods. The methods were ideally suited to the cornea images and for fluorescein stained corneal defects in particular.
Example 4 Polar Filtering Eliminates Specular Images Reflecting from the Ocular Surface
The need to remove specular images of the illumination source from ocular surface images is not limited to fluorescein stained eyes. During the course of several other ocular examinations, such as measuring hyperemia or colored conjunctival stains, such as lissamine green or rose bengal, it would be advantageous to remove the specular images of the source to facilitate subsequent analysis. For non-fluorescent imaging, polarization optics can be used to filter specular reflected light from ocular images. An example of this is shown in FIG. 7
FIG. 7A shows an image of an ocular surface obtained by illuminating with left circularly polarized light using a ring light source and imaged without a polar filter in the eye to camera light path. The specular image of the ring light appeared as a bright white ring in the center of the eye (FIG. 7A). FIG. 7B, shows an image of the ocular surface illuminated with left circular polarized light using the same ring light source and imaged through a right circular polar filter in the eye to camera light path. The specular reflected light from the ring light was blocked by the cross polar filter and the image was free of specular artifact (FIG. 7B). Thus, polarized light filtering eliminated the Purkinje artifacts from the ocular surface image.
It should be understood that the foregoing disclosure emphasizes certain specific embodiments of the invention and that all modifications or alternatives equivalent thereto are within the spirit and scope of the invention as set forth in the appended claims.
Claims
1. A method of detecting an ocular surface disease, the method comprising: a. illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is transmitted in a first predetermined wavelength range by an illumination filter positioned between the light source and the ocular surface, and wherein the light in the first predetermined wavelength range excites a contrast agent bound to defects on the ocular surface; and b. detecting a light signal emitted from the contrast agent, wherein the light signal is transmitted in a second predetermined wavelength range by an imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device; wherein the image capture device transmits signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution.
2. The method of Claim 1, wherein the ocular surface disease is dry eye.
3. The method of Claim 1, wherein the optical density of the illumination filter at wavelengths other than the first predetermined wavelength range is less than or equal to 0.000001 and the optical density of the imaging filter is less than or equal to 0.000001 at wavelengths other than the second predetermined wavelength range.
4. The method of Claim 1, wherein the contrast agent is fluorescein, the illumination filter transmits light in a range of 465 to 500 nm, and the imaging filter transmits light greater than 515 nm.
5. A method of detecting an ocular surface disease, the method comprising: a. illuminating the ocular surface of an eye of a patient with a light from a light source, wherein the light is polarized in a first orientation by an illumination filter positioned between the light source and the ocular surface, and wherein the light polarized in the first orientation excites a contrast agent bound to defects on the ocular surface; and b. detecting a light signal emitted from the contrast agent, wherein the light signal is polarized in a second orientation by an imaging filter, and is transmitted by the imaging filter to an image capture device, wherein the imaging filter is positioned between the ocular surface and the image capture device; wherein the image capture device transmits signals to a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution.
6. The method of Claim 5, wherein the illumination filter and the imaging filter are polar filters, and are adjusted in opposite directions.
7. The method of Claim 5, wherein the illumination filter and the imaging filter are circular polar filters, and wherein one of the filters is left circular and the other is right circular.
8. An ocular surface examination apparatus, comprising: a. a light source for directing light along an illumination path onto an ocular surface; b. an illumination filter that transmits light in the illumination path; c. an imaging filter that transmits light reflected from a contrast agent on the ocular surface of a patient along an imaging path; and d. an image capture device for detecting light reflected from the contrast agent on the ocular surface of the patient; and e. an optical system to increase depth of field in the captured image; wherein the light in the illumination path cannot pass through the imaging filter.
9. The apparatus of Claim 8, further comprising a machine readable storage medium comprising instructions that provide quantitative analysis of contrast agent intensity and distribution.
10. The apparatus of Claim 8, wherein the illumination filter transmits light in a first predetermined wavelength range, and the imaging filter transmits light in a second predetermined wavelength range, wherein the first and second predetermined wavelength ranges do not overlap.
11. The apparatus of Claim 10, wherein the illumination filter transmits light in a range of 465 to 500 nm, and the imaging filter transmits light greater than 515 nm.
12. The apparatus of Claim 10, wherein the optical density of the illumination filter at wavelengths other than 465 to 500 nm is less than or equal to 0.000001 and the optical density of the imaging filter is less than or equal to 0.000001 at wavelengths between 465 to 500 nm.
13. The apparatus of Claim 8, wherein the illumination filter and the imaging filter are polar filters, and are adjusted in opposite directions.
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Cited By (3)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US8923578B2 (en) | 2010-05-06 | 2014-12-30 | Alcon Research, Ltd. | Devices and methods for assessing changes in corneal health |
US9232889B2 (en) | 2009-02-12 | 2016-01-12 | Alcon Research, Ltd. | Method and apparatus for ocular surface imaging |
US9241622B2 (en) | 2009-02-12 | 2016-01-26 | Alcon Research, Ltd. | Method for ocular surface imaging |
Families Citing this family (26)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US8574277B2 (en) * | 2009-10-21 | 2013-11-05 | Avedro Inc. | Eye therapy |
JP6377906B2 (en) | 2010-03-19 | 2018-08-22 | アヴェドロ・インコーポレーテッドAvedro,Inc. | System for applying and monitoring eye treatment |
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CA3113120A1 (en) | 2018-10-09 | 2020-04-16 | Avedro, Inc. | Photoactivation systems and methods for corneal cross-linking treatments |
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Citations (8)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US5852498A (en) * | 1997-04-04 | 1998-12-22 | Kairos Scientific Inc. | Optical instrument having a variable optical filter |
US5986271A (en) * | 1997-07-03 | 1999-11-16 | Lazarev; Victor | Fluorescence imaging system |
US6044196A (en) * | 1992-03-23 | 2000-03-28 | Minnesota Mining & Manufacturing, Co. | Luminaire device |
US6049367A (en) * | 1995-05-23 | 2000-04-11 | Colorlink, Inc. | Polarization manipulating device modulator with retarder stack which preconditions light for modulation and isotropic states |
US20020151774A1 (en) * | 2001-03-01 | 2002-10-17 | Umass/Worcester | Ocular spectrometer and probe method for non-invasive spectral measurement |
US20060077581A1 (en) * | 2004-08-31 | 2006-04-13 | Jim Schwiegerling | Multipurpose optical imaging device, system and method |
US20080090198A1 (en) * | 2006-10-13 | 2008-04-17 | Rongguang Liang | Apparatus for caries detection |
US20080239070A1 (en) * | 2006-12-22 | 2008-10-02 | Novadaq Technologies Inc. | Imaging system with a single color image sensor for simultaneous fluorescence and color video endoscopy |
Family Cites Families (34)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
JPH06277179A (en) * | 1993-01-28 | 1994-10-04 | Kowa Co | Ophthalmic measuring apparatus |
JP3340805B2 (en) | 1993-07-27 | 2002-11-05 | 興和株式会社 | Ophthalmic measurement device |
US6252979B1 (en) * | 1995-06-07 | 2001-06-26 | Tripath Imaging, Inc. | Interactive method and apparatus for sorting biological specimens |
US5924487A (en) | 1997-01-31 | 1999-07-20 | Halliburton Energy Services, Inc. | Proppant slurry screen apparatus and methods of using same |
US6024449A (en) * | 1998-07-13 | 2000-02-15 | Smith; Robert F. | High speed topography measurement of semi-diffuse objects |
US6006756A (en) | 1998-08-03 | 1999-12-28 | Shadduck; John H. | Non-contact magnetoresonant implant system and techniques for periodic corneal re-shaping |
JP3699853B2 (en) * | 1999-02-18 | 2005-09-28 | 株式会社ニデック | Ophthalmic equipment |
JP2000296109A (en) | 1999-04-15 | 2000-10-24 | Canon Inc | Optometer |
GR1004180B (en) * | 2000-03-28 | 2003-03-11 | ����������� ����� ��������� (����) | Method and system for characterization and mapping of tissue lesions |
WO2004111621A1 (en) * | 2003-06-19 | 2004-12-23 | Koninklijke Philips Electronics N.V. | Analysis apparatus and method comprising auto-focusing means |
CN1833257A (en) | 2003-07-09 | 2006-09-13 | 仁爱米拉索莱有限公司 | Method and apparatus for analyzing biological tissues |
US7346203B2 (en) | 2003-11-19 | 2008-03-18 | General Electric Company | Methods and apparatus for processing image data to aid in detecting disease |
US7338167B2 (en) * | 2003-12-10 | 2008-03-04 | Joslin Diabetes Center, Inc. | Retinal imaging system |
WO2006047475A2 (en) * | 2004-10-25 | 2006-05-04 | Sytera, Inc. | Detection and analysis of ophthalmically-relevant fluorescent molecules |
DE102005026371B4 (en) | 2005-06-07 | 2024-02-08 | Oculus Optikgeräte GmbH | Method for operating an ophthalmological analysis system |
DE102005034332A1 (en) * | 2005-07-22 | 2007-01-25 | Carl Zeiss Meditec Ag | Apparatus and method for observation, documentation and / or diagnosis of the ocular fundus |
JP5114024B2 (en) | 2005-08-31 | 2013-01-09 | オリンパス株式会社 | Optical imaging device |
US7778491B2 (en) * | 2006-04-10 | 2010-08-17 | Microsoft Corporation | Oblique image stitching |
EP2656780B1 (en) | 2006-05-26 | 2016-04-27 | The Cleveland Clinic Foundation | System for measuring biomechanical properties in an eye |
US20080077581A1 (en) | 2006-09-25 | 2008-03-27 | Jay Drayer | System and method for providing medical disposition sensitive content |
AU2007319374B2 (en) | 2006-11-10 | 2012-07-12 | Amo Manufacturing Usa, Llc | Operator-controlled scanning laser procedure designed for large-area epithelium removal |
JP2008264137A (en) | 2007-04-18 | 2008-11-06 | Topcon Corp | Cornea observation apparatus |
US7860286B2 (en) * | 2007-04-24 | 2010-12-28 | Microsoft Corporation | Medical image acquisition error detection |
JP5160826B2 (en) | 2007-07-19 | 2013-03-13 | 株式会社トプコン | Corneal observation device |
WO2009124271A1 (en) | 2008-04-03 | 2009-10-08 | Arcscan, Inc. | Procedures for an ultrasonic arc scanning apparatus |
US9039623B2 (en) | 2008-05-29 | 2015-05-26 | Arcscan, Inc. | Compound scanning head for an ultrasonic scanning apparatus |
US20100079580A1 (en) | 2008-09-30 | 2010-04-01 | Waring Iv George O | Apparatus and method for biomedical imaging |
WO2010079580A1 (en) | 2009-01-09 | 2010-07-15 | Ntn株式会社 | Microinjection apparatus and microinjection method |
US9241622B2 (en) | 2009-02-12 | 2016-01-26 | Alcon Research, Ltd. | Method for ocular surface imaging |
EP2395906A4 (en) | 2009-02-12 | 2017-06-28 | Novartis Ag | Method and apparatus for ocular surface imaging |
JP5733962B2 (en) | 2010-02-17 | 2015-06-10 | キヤノン株式会社 | Ophthalmologic apparatus, ophthalmologic apparatus control method, and program |
US8414564B2 (en) | 2010-02-18 | 2013-04-09 | Alcon Lensx, Inc. | Optical coherence tomographic system for ophthalmic surgery |
US20110271470A1 (en) | 2010-05-04 | 2011-11-10 | Baker Hughes Incorporated | Brush Assembly with Non-Rotating Stabilizer and Brushes |
WO2011139827A1 (en) | 2010-05-06 | 2011-11-10 | Alcon Research, Ltd. | Devices and methods for assessing changes in corneal health |
-
2010
- 2010-02-11 EP EP10741709.9A patent/EP2395906A4/en not_active Withdrawn
- 2010-02-11 US US12/704,083 patent/US9232889B2/en active Active
- 2010-02-11 JP JP2011550224A patent/JP5628839B2/en not_active Expired - Fee Related
- 2010-02-11 WO PCT/US2010/023865 patent/WO2010093772A1/en active Application Filing
Patent Citations (8)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US6044196A (en) * | 1992-03-23 | 2000-03-28 | Minnesota Mining & Manufacturing, Co. | Luminaire device |
US6049367A (en) * | 1995-05-23 | 2000-04-11 | Colorlink, Inc. | Polarization manipulating device modulator with retarder stack which preconditions light for modulation and isotropic states |
US5852498A (en) * | 1997-04-04 | 1998-12-22 | Kairos Scientific Inc. | Optical instrument having a variable optical filter |
US5986271A (en) * | 1997-07-03 | 1999-11-16 | Lazarev; Victor | Fluorescence imaging system |
US20020151774A1 (en) * | 2001-03-01 | 2002-10-17 | Umass/Worcester | Ocular spectrometer and probe method for non-invasive spectral measurement |
US20060077581A1 (en) * | 2004-08-31 | 2006-04-13 | Jim Schwiegerling | Multipurpose optical imaging device, system and method |
US20080090198A1 (en) * | 2006-10-13 | 2008-04-17 | Rongguang Liang | Apparatus for caries detection |
US20080239070A1 (en) * | 2006-12-22 | 2008-10-02 | Novadaq Technologies Inc. | Imaging system with a single color image sensor for simultaneous fluorescence and color video endoscopy |
Non-Patent Citations (1)
Title |
---|
See also references of EP2395906A4 * |
Cited By (3)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
US9232889B2 (en) | 2009-02-12 | 2016-01-12 | Alcon Research, Ltd. | Method and apparatus for ocular surface imaging |
US9241622B2 (en) | 2009-02-12 | 2016-01-26 | Alcon Research, Ltd. | Method for ocular surface imaging |
US8923578B2 (en) | 2010-05-06 | 2014-12-30 | Alcon Research, Ltd. | Devices and methods for assessing changes in corneal health |
Also Published As
Publication number | Publication date |
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JP2012517325A (en) | 2012-08-02 |
EP2395906A4 (en) | 2017-06-28 |
EP2395906A1 (en) | 2011-12-21 |
US20100204584A1 (en) | 2010-08-12 |
US9232889B2 (en) | 2016-01-12 |
JP5628839B2 (en) | 2014-11-19 |
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