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WO2000069333A1 - Detection optique de maladies dentaires au moyen d'une lumiere polarisee - Google Patents

Detection optique de maladies dentaires au moyen d'une lumiere polarisee Download PDF

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Publication number
WO2000069333A1
WO2000069333A1 PCT/US2000/013878 US0013878W WO0069333A1 WO 2000069333 A1 WO2000069333 A1 WO 2000069333A1 US 0013878 W US0013878 W US 0013878W WO 0069333 A1 WO0069333 A1 WO 0069333A1
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recited
light
depolarization
polarization
dental tissue
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English (en)
Inventor
Matthew J. Everett
Billy W. Colston, Jr.
Ujwal S. Sathyam
Luiz B. Da Silva
Daniel Fried
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University of California Berkeley
University of California San Diego UCSD
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University of California Berkeley
University of California San Diego UCSD
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Priority to AU51476/00A priority Critical patent/AU5147600A/en
Publication of WO2000069333A1 publication Critical patent/WO2000069333A1/fr
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B5/00Measuring for diagnostic purposes; Identification of persons
    • A61B5/0059Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence
    • A61B5/0082Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence adapted for particular medical purposes
    • A61B5/0088Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence adapted for particular medical purposes for oral or dental tissue
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B5/00Measuring for diagnostic purposes; Identification of persons
    • A61B5/0059Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence
    • A61B5/0062Arrangements for scanning
    • A61B5/0066Optical coherence imaging
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61BDIAGNOSIS; SURGERY; IDENTIFICATION
    • A61B5/00Measuring for diagnostic purposes; Identification of persons
    • A61B5/0059Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence
    • A61B5/0073Measuring for diagnostic purposes; Identification of persons using light, e.g. diagnosis by transillumination, diascopy, fluorescence by tomography, i.e. reconstruction of 3D images from 2D projections
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01BMEASURING LENGTH, THICKNESS OR SIMILAR LINEAR DIMENSIONS; MEASURING ANGLES; MEASURING AREAS; MEASURING IRREGULARITIES OF SURFACES OR CONTOURS
    • G01B9/00Measuring instruments characterised by the use of optical techniques
    • G01B9/02Interferometers
    • G01B9/0209Low-coherence interferometers
    • G01B9/02091Tomographic interferometers, e.g. based on optical coherence
    • GPHYSICS
    • G01MEASURING; TESTING
    • G01BMEASURING LENGTH, THICKNESS OR SIMILAR LINEAR DIMENSIONS; MEASURING ANGLES; MEASURING AREAS; MEASURING IRREGULARITIES OF SURFACES OR CONTOURS
    • G01B2290/00Aspects of interferometers not specifically covered by any group under G01B9/02
    • G01B2290/70Using polarization in the interferometer

Definitions

  • the present invention relates to the detection of dental disease using polarized light by optically measuring the depolarization of incident light backscattered from dental tissues.
  • Dental caries or tooth decay, is a pathological process of destruction of tooth structure by oral microorganisms, which can lead to tooth loss if untreated.
  • coronal caries lesions begin in the enamel and cause demineralization of the enamel. This demineralization changes the scattering properties of the enamel, resulting in chalky or "white spot" lesions visible when the caries occurs on smooth, unstained enamel surfaces. If the carious lesion is detected before it reaches the dentin, remineralization is still possible. After the carious lesion has reached dentin, however, inflammation of the pulp occurs, requiring a filling and leading to serious tooth decay and eventual tooth loss if untreated. Restorative dentistry is most effective when the progression of caries is detected early before it reaches the dentin.
  • Radiography is often used for detection of cavities, since it provides integrated views of tooth structure that in certain orientations can isolate carious lesions.
  • the sensitivity of radiographic systems is limited by visible changes in film density, making identification of small carious or precarious regions difficult. Since radiographs are two dimensional, precisely locating the position of such decay is impossible.
  • radiography due to the orientation of the x-ray imaging, only interproximal lesions (between the teeth) are easily detected, while early occlusal lesions (top of the tooth), are difficult to detect.
  • radiography uses harmful ionizing radiation.
  • This invention applies the technique of polarimetry to image dental hard tissue and detect the presence of caries based on the depolarization of incident light.
  • the invention also has the potential for detection of disease in bone.
  • Polarimetry is a well-established tool for non-invasive material characterization and involves comparison of the polarization states of light before and after the light interacts with the material.
  • the use of polarized light for characterization and imaging of highly scattering media, such as biological tissue, has been studied.
  • the effect of scattering on the polarization state of li ht has been found to be useful for imaging of surface or subsurface structures in scattering media, and for transmission imaging of deep structures.
  • Optical coherence-domain reflectometry a new optical evaluation technique
  • the first fiber optic based OCDR system was constructed by the U.S. National Bureau of Standards for micro-optic technology. See Danielson et al, "Guided- wave reflectometry with micrometer resolution", Applied Optics 26(14):2836-2842 (1987).
  • OCDR uses a low coherence Michelson interferometer to probe the sample, generating reflection signals as a function of depth. When the probe beam is transversed across the sample, a series of axial scans can be stacked together to form a high-resolution two-dimensional optical coherence tomogram. See Lee et. al, "Profilometry with a coherence scanning microscope", Applied
  • OCT optical coherence tomography
  • PS-OCT has also been used for measuring birefringence in teeth in an unsuccessful attempt at caries detection. This attempt was unsuccessful because caries causes light to become depolarized by changing the scattering coefficient of the enamel rather than significantly affecting the birefringence of the enamel. See Baumgartner et al., "Optical coherence tomography of dental structures", Proc. SPIE 3248; Lasers in Dentistry IV, John D. Featherstone, Peter Rechmann, Daniel S. Fried, eds., pp. 130-136 (1998).
  • No. 09/315,000 assigned to the same assignee, describes a dental explorer device for detecting caries and periodontal disease using OCDR, and is incorporated herein by reference.
  • an OCDR dental device was developed in the form of a hand-held, portable explorer tool for non-invasively probing teeth and other dental tissues.
  • the OCDR explorer was designed to safely and accurately collect intraoral OCT images of dental tissue and microstrucrure in vivo for evaluation of dental health.
  • the capabilities of the dental explorer device have been further expanded and improved in the present invention by the incorporation of polarization sensitive diagnostics.
  • the invention uses PS-OCT to measure the depolarization of light associated with optical scattering, rather than changes in polarization state associated with birefringence, to detect demineralization and caries.
  • This invention provides an optical technique and dental tool that use polarized light for early, non-invasive, and effective diagnosis of the state and structure of hard biological tissues (e.g., teeth and bone).
  • the invention is particularly suited for detection of precarious and carious lesions, and may be useful for evaluation of dental restorations.
  • the method is based on optically detecting the change in polarization of the incident light backscattered from dental tissues.
  • the demineralization of tooth enamel that is the precursor to caries disease modifies the scattering properties of the tissue, resulting in depolarization of the incident light, which is then detected by the optical imaging system.
  • the tooth (or other mineralized tissue) is irradiated with polarized light having a selected or known polarization state, either circular, linear, or elliptical. Light backscattered from the tooth is then analyzed using optical polarimetry to determine its degree of polarization.
  • the tooth can also be irradiated with multiple polarization states sequentially to differentiate between changes in polarization state associated with birefringence and depolarization. Depth-resolved images of the demineralization of the enamel can be obtained based on either the temporal or spatial coherence of the incident light by using optical coherence domain reflectometry or confocal imaging, respectively, and incorporating polarimetry. Depth-resolved information about the depolarization is useful as it enables identification of subsurface precarious and carious lesions and minimizes the effects of fresnel reflections from the front surface of the tooth, which can make the results more difficult to interpret.
  • the polarization sensitive optical imaging system can incorporate a dental explorer tool, which contains one or more optical fibers that independently couple light from the optical imaging system to the tip of a dental probe.
  • the probe is placed against the tooth (or hard tissue), and light from the fiber at the tip of the probe is directed into the enamel.
  • the light reflected or backscattered from the tissue is then collected by an optical fiber and detected by the optical imaging system.
  • the polarized light is delivered and collected using a polarization sensitive OCDR system, which provides a single point profile of optical scattering (and thus tissue microstructure) as a function of depth.
  • the OCDR system consists of a light source split by a beamsplitter or fiber optic coupler into a sample arm and reference arm. Reflected or backscattered light from the tissue is collected in the sample arm and detected by heterodyning with the light in the reference arm. Only the photons in the sample arm that have traveled the same optical path length as the photons in the reference arm (within the coherence length of the source) generate a heterodyne signal. Thus, by varying the path length of the reference beam and recording the amplitude of the heterodyne signal, the
  • OCDR system measures the scattering coefficient of the tissue as a function of depth. By moving the dental probe transversely across the tissue, the clinician can obtain a series of profiles of tissue microstructure. These profiles are combined to form a cross- sectional, or optical coherence tomography (OCT), image of the region of interest in the oral cavity.
  • OCT optical coherence tomography
  • the polarization sensitive OCDR/OCT systems provide images of polarization state as a function of depth.
  • the object of this invention is to provide a dental tool that uses the depolarization of incident light to detect changes in the tissue microstructure that are indicative of disease.
  • Another object of the invention is to provide a dental tool that combines polarimetry and optical coherence domain reflectometry. It is further an object of this invention to combine polarimetry with optical coherence tomography to generate depth-resolved images of the degree of polarization of light passing through tissue as a function of tissue depth.
  • the invention uses PS-OCT to measure the depolarization of light associated with optical scattering, rather than effects due to birefringence. This invention is particularly suited to detecting the demineralization of teeth associated with caries, and may be useful for detecting demineralization of other mineralized tissues, such as bone.
  • Figure 1 shows a polarimetric imaging system used in the present invention.
  • Figure 2 shows a polarization sensitive optical imaging system using optical coherence domain reflectometry with bulk optics.
  • Figure 3 shows a fiber optic based polarization sensitive optical imaging system used in the present invention.
  • Figure 4 shows an embodiment of a hand-held fiber optic dental probe according to the present invention.
  • Figure 5 shows an embodiment of an optical polarimetry imaging system used in the present invention.
  • Figure 6 shows a plot of extinction ratio as a function of transverse position for demineralized tooth enamel and normal enamel.
  • the present invention is a dental tool and optical method for detection of caries by measuring the depolarization of light backscattered from hard dental tissue, such as enamel.
  • Polarized light is directed at the dental tissue to be examined, and the light backscattered from the tissue is then collected and the change in its polarization state measured.
  • the polarization state of the backscattered or reflected light can be analyzed either using optical polarimetric imaging techniques or using polarization sensitive optical coherence domain reflectometry (PS-OCDR) and optical coherence tomography (PS-OCT) systems, which measure the depolarization as a function of tissue transverse position and depth.
  • PS-OCDR polarization sensitive optical coherence domain reflectometry
  • PS-OCT optical coherence tomography
  • the light used for probing the dental tissue is in the visible or near- infrared (e.g., >700 nm), thus avoiding the ionizing radiation used in radiography.
  • the present invention is particularly useful for detecting precarious and carious lesions.
  • An indicator of caries is demineralization of the enamel, which causes large-angle scattering and changes the scattering coefficient of the enamel. This scattering affects the polarization state of the light scattered or reflected back from the tooth. Specifically, light scattered from normal enamel remains polarized, while light scattered from demineralized enamel becomes depolarized.
  • the invention measures the polarization state, or amount of depolarization, of the backscattered light, thereby detecting the degree of demineralization in the enamel.
  • Optical polarimetry using a CCD camera and polarizers is useful for imaging of surface caries and images a number of teeth simultaneously, while PS-OCDR or PS-OCT systems provide depth resolution, improving the sensitivity of the system to caries and enabling identification of subsurface demineralization sites. Depth- resolved imaging can also be achieved through confocal imaging. Confocal optical imaging systems are known in the art (e.g., see U.S. Patent RE32,660 to Lindow et al . ) .
  • Figure 1 shows an embodiment of a polarimetric imaging system used in accordance with the present invention.
  • the sample 10 such as a tooth
  • the sample 10 is illuminated by a low coherence light source 12 followed by a polarizer 14, an optional wave plate 16, and a collimating lens 18.
  • the polarizer 14 and collimator 18 cause an incident beam of polarized light to be focused on the sample 10, while the wave plate 16 makes the polarization state adjustable.
  • the incident beam has a known polarization state. Any polarization state can be used: circularly polarized, elliptically polarized, or linearly polarized. A series of different incident polarization states can also be used sequentially.
  • the use of a series of polarization states makes it possible to discriminate the changes in polarization associated with depolarization from birefringence-induced polarization changes.
  • the reflected scattered light from the illuminated sample 10 passes through a wave plate 20 and polarizer 22, and then is imaged onto a detector 24, such as a CCD camera or photodetector.
  • An optional optical bandpass filter 26 may be inserted after the polarizer 22, as shown.
  • the bandpass filter 26 is used to select the wavelength band for optimum discrimination between normal enamel and carious lesions.
  • the polarizer /wave plate combination selects the appropriate polarization states to be detected by the detector 24.
  • the sample is imaged twice by the detector 24, once with the polarizer 22 in front of the detector 24 oriented to pass horizontally polarized light, and once with the polarizer 22 passing vertically polarized light.
  • the two polarization states could also be measured simultaneously, using two detectors or CCD cameras.
  • the two images are processed by an analyzer 28, which includes a computer.
  • a third image is generated by the analyzer 28, which displays the amount of depolarization occurring at each location on the surface of each sample, by taking the ratio or a related mathematical function of the two images (for instance, the difference of the two images over the sum of the two images).
  • FIG. 2 shows an embodiment of a polarimetric, depth- resolved optical imaging system based on OCDR/OCT using bulk optics.
  • This system has a light source 30 that produces an incident beam of light that is collimated using optics 32 and polarized by a polarizer 34.
  • the source 30 is typically a broad bandwidth (on the order of 50 nm) amplified spontaneous emission (ASE) source such as a superluminescent diode or fiber ASE source operating in the visible or near infrared.
  • ASE amplified spontaneous emission
  • the polarized light is split by a non- polarizing beamsplitter 36 into a reference arm 38 and a sample arm 40 of a Michelson interferometer.
  • the sample beam may pass through a wave plate 42 and optics 44 before illuminating the area of interest on the sample 46.
  • the wave plate 42 (or retardation plate) in the sample arm 40 controls the state of polarization of the light incident on the sample 46 and makes it possible to illuminate the sample with a series of different polarization states sequentially.
  • the reference arm 38 provides a variable optical delay.
  • the reference beam is directed to a reference mirror 48, which is translated in the direction of beam propagation to vary the path length.
  • the reflected beam from the reference mirror 48 and the backscattered light from the sample 46 are recombined by the beamsplitter 36.
  • a polarizing cube (or beamsplitter) 50 splits the recombined beam into its horizontal and vertical polarization components, which are then focused by optics 52 and coupled by single mode fibers onto two photodetectors 54.
  • a quarter-wave plate 56 set at 22.5° to the horizontal in the reference arm 38 rotates the linear polarization of the returning light by 45° such that it is split evenly between the two detectors 54. This quarter-wave plate could be replaced with any polarizing optic which causes equal amounts of light to be in the vertical and horizontal polarization states.
  • the information recorded by the detectors 54 is then processed by an analyzer 62.
  • Depolarization is quantified by the analyzer by measuring the relative intensities of the heterodyned signals in the two orthogonal polarization states.
  • Backscattered light from the tissue is collected in the sample arm and measured as a function of depth in the tissue by varying the reference arm path length while the measuring the heterodyne signal.
  • a heterodyne signal is generated when the light in the sample arm has traveled the same optical path length as the light in the reference arm within the coherence length of the source.
  • the OCDR system measures the amount of light backscattered from the tissue and its polarization state as a function of transverse position and depth.
  • transverse scanning results in a polarization-sensitive OCT system, generating two-dimensional cross-sectional maps of the polarization state of the light within the sample.
  • a series of one-dimensional scans are combined to create two-dimensional intensity and polarization plots.
  • the acquisition times for cross-sectional images are less than one minute, and typically on the order of seconds. This approach provides depth- resolved information about depolarization and therefore facilitates the identification of subsurface sites of demineralization.
  • Transverse scanning mechanisms are described in co-pending U.S. patent application, Hand-Held Dental Imaging Device, Serial No. 60/116885, co-assigned to the same assignee, which is incorporated herein by reference.
  • An alternative embodiment of the polarization sensitive OCDR/OCT system would eliminate the axial scanning, and instead simply modulate the pathlength of the reference arm a distance on the order of a few microns or less. This system would then measure the depolarization of the incident light backscattered from a fixed depth in the tissue.
  • the OCDR/OCT system described above for Figure 2 is a bulk optic system and therefore not easily deployable for in vivo use in a dental office.
  • a more practical system offers ease of use and portability, such as a fiber optic based system.
  • a fiber optic polarization sensitive OCDR/OCT system follows the same principles as the system shown in Figure 2, but using polarization maintaining (PM) fibers and replacing most of the bulk optic components with in-line fiber optic components.
  • Figure 3 shows a diagram of a fiber optic based polarization- sensitive OCDR/OCT system suitable for in vivo measurements.
  • the bulk optic polarizers and beamsplitter shown in Figure 2 are replaced with an in-line fiber optic coupler or beamsplitter and inline polarizers, and the free space between the components replaced with PM optical fiber 58.
  • the reference arm length can be varied with a retro-reflector (or mirror) 60 driven by a galvanometer.
  • the detectors, wave plates, and collimating lenses remain the same as in Figure 2.
  • the only significant alignment required is the coupling of light from the reference arm fiber onto the retro-reflector 60 and then back into the fiber. Even this bulk optic reference arm can be eliminated by using a piezoelectric transducer system to vary the length of the reference arm fiber and/or the sample arm fiber.
  • the fiber optic based system ensures that the detectors 54 collecting the two polarization states are always identically aligned for the light reflected from the reference arm and the sample arm, greatly enhancing the reliability and ease of use of the system. In addition to improving the reliability of the system, these changes make it possible to use the system for in vivo measurements, as it is possible to use an optical fiber to probe the oral cavity.
  • FIG 4 shows an embodiment of a hand-held fiber optic dental probe according to the present invention.
  • the probe incorporates an optical fiber that couples to an imaging system, such as a polarimetric imaging system as shown in Figure 1 having polarizers and a CCD camera.
  • the dental probe optical fiber is the sample arm coupled to a PS-OCDR/OCT system, as shown in Figures 2-3.
  • the OCDR/OCT system provides depth- resolved detection of diseased (e.g., carious) lesions wherever the tip of the probe touches the sample tissue (e.g., a tooth).
  • This fiber optic probe for in vivo diagnosis of caries resembles a dental explorer, a device familiar to dental clinicians.
  • the device 70 comprises a hand-held portion 72 so that the operator can manually manipulate the device, and a probe portion 74 that can be easily inserted into a patient' s mouth.
  • the device can be designed so that the probe is manipulated robotically or remotely, in which case a handle for an operator is unnecessary.
  • the shape of the probe portion 74 is designed to comfortably access as much of the oral cavity as possible, and thus may be curved or angled like a conventional dental explorer so that the tip 76 of the probe reaches the posterior portions of the dental cavity.
  • the bends or curves in the probe and optical fiber are limited by the radius of curvature at which significant amounts of light escape from the fiber, typical approximately 0.5 cm.
  • the device 70 contains a single mode polarization maintaining (PM) optical fiber 78, which independently couples light from an imaging system 80 to the tip 76 of the explorer device 70. Light is emitted from the tip 76 of the device 70 from the distal end of the fiber 78. An optional miniature waveplate can be attached to the end of the fiber to cause the linearly polarized light from the fiber to become circularly polarized. Alternatively, a polarization maintaining (PM) optical fiber can be used, and the fiber can be rotated or twisted to vary the polarization. The rotation can be effected by manually rotating the explorer device or by mechanical means within the explorer device connected to the fiber. When the imaging system is an OCDR/OCT system, the device serves as an extension of the sample arm, and the system provides depth- resolved detection of carious lesions wherever the tip of the explorer device touches a tooth.
  • PM polarization maintaining
  • references to a single fiber also extend to the use of a plurality of fibers.
  • the light from the tip of the device is emitted from the distal end of a plurality of fibers.
  • the fiber optic bundle is connected to an optical switch 82 or optical multiplexer, which is used to switch light between the fibers in the bundle.
  • the optical switch 82 is connected to the imaging system 80.
  • each fiber is connected to separate imaging systems 80.
  • the probe light emitted from the distal end of the fiber 78 is emitted from the tip 76 of the explorer device 70 and directed at or into the hard tissue, such as enamel, at the appropriate location.
  • the probe tip 76 may be placed next to a tooth, or slipped between a tooth and periodontal tissue.
  • the spot size is typically less than 50 ⁇ m, and can be on the order of 5 ⁇ m.
  • the distal end of the fiber is cut and/or polished at an angle, typically approximately 10 degrees, to eliminate back reflections.
  • the light can also be directed to the tissue through the side of the fiber and probe by angle-polishing the fiber tip at a steeper angle, i.e., near 45 degrees, and then coating the polished surface with a metal such as aluminum.
  • the probe light which would have been emitted out the end of the fiber 78, is then reflected, thus imaging the tissue next to the fiber tip instead of in front of it.
  • the light may be focused using one or more small diameter (e.g., millimeter or submillimeter) optical elements or optics, such as gradient index (GRIN) lenses, mirrors, or prisms.
  • the focusing /collection optics may be mounted or attached directly to the end of the PM fiber, or the light may travel through free space from the PM fiber to the optics. If a lens is mounted to the end of the fiber, an index matching ultraviolet curable epoxy may be placed at the fiber /lens interface to minimize refractive index mismatch and reflections.
  • the probe can be constructed to direct the polarized light at any angle or angles relative to the tip.
  • the light is emitted substantially parallel to the fiber, from the very tip of the probe portion.
  • the device can be "side-firing", where the light is emitted from the side of the tip.
  • the light may be redirected or focused to the appropriate location by angle-polishing the end of the fiber or by using small (submillimeter diameter) focusing /collection optics, such as a GRIN lens and/or a prism.
  • the optics may be attached directly to the PM fiber using an index-matching epoxy.
  • the device tip can also be designed to permit light to be emitted from one or more PM fibers in one or more directions at the tip or through a plurality of openings or transparent areas at or near the tip.
  • the fiber and focusing /collection optics are preferably internal to the handle and probe portions of the explorer device.
  • the probe portion may be a small diameter hollow tube, tapering like a needle at the tip.
  • the light emitted from the end of the fiber may pass through an uncovered opening at or near the tip of the device, or through an opening covered by a window of transparent material, or the tip or probe portion may be made of a transparent material. Since the tip of the probe is in contact with dental tissues and fluids, the tip or probe portion must be detachable and disposable, or capable of being sterilized. Suitable materials for making the probe tip include glass and metals. Alternatively, a transparent, sterilized, disposable cover piece for hygienic purposes can be placed over the tip of the probe portion before insertion into the patient' s oral cavity.
  • the polarized incident beam interacts with the sample (e.g., tooth)
  • the light reflected or backscattered from the tissue is then collected by the same optical fiber and detected by the imaging system 80.
  • the information i.e., the amount of depolarization, is then processed by an analyzer 84.
  • the images processed by the analyzer may be displayed on a video display monitor 86 for visual inspection.
  • the 84 may be programmed to send a signal when the depolarization of the illuminated tissue is within a selected range of values to alert the clinician that diseased tissue may be present.
  • the signal could be auditory, such as a series of beeps, or in the form of a visual display.
  • each measurement provides a single point profile of optical scattering and polarization state as a function of depth.
  • a series of profiles of tissue microstructure are generated.
  • the collected one- dimensional scans are combined by the analyzer to form a depth- resolved, two-dimensional, cross-sectional OCT image of the polarization state of light backscattered from the tooth.
  • EXAMPLE I A prototype optical polarimetry system as shown in Figure 5 was built and tested to detect caries using the polarization state of light backscattered from enamel.
  • the fiber coupled source is indicated at 90, lenses are indicated at 92, polarizers are indicated at 94, the sample is indicated at 96, a half-wave plate is indicated at 98, the beamsplitter is indicated at 100, the detector is indicated at 102, and the analyzer to process the data and associated images is indicated at 104.
  • the source was a horizontally polarized superluminescent diode operating at a center wavelength of 1310 nm, with a spectral band of 47 nm.
  • the sample consisted of two juxtaposed 5 mm wide blocks of porcine enamel, one of which was artificially demineralized using an acid bath. The two blocks were oriented at 20 degrees to the normal in the vertical plane to eliminate specular reflections.
  • a bulk optic polarization-sensitive OCT (PS-OCT) system as shown in Figure 2 was built and tested to generate cross-sectional images of carious lesions.
  • the PS-OCT system used a 15 mW superluminescent diode source operating at a center wavelength of 1310 nm, with a spectral bandwidth of 47 nm (FWHM) which was passed through a polarizer, providing 7.5 mW of horizontally polarized light.
  • FWHM spectral bandwidth
  • the sample was scanned transversely across the incident beam from the normal enamel surface to the demineralized area, and the longitudinal scans at each transverse position were combined to generate a two-dimensional OCT map of the polarization state of the returning light.
  • the two heterodyned signals can also be combined to generate a polarization-insensitive intensity map.
  • the data showed that although the backscattering intensity was only slightly affected by the demineralization, the polarization state of the scattered light clearly delineated the normal enamel from the carious region due to depolarization.
  • the polarization-sensitive OCT system was applied to scanning extracted human teeth containing naturally occurring carious lesions in the enamel. The images generated were compared to histological sections of the relevant areas of the tooth. The carious enamel was clearly delineated by the polarization state of the scattered light. Both the histology and the polarization image showed demineralized enamel in the same regions. Vertical stripes seen in the images in the normal enamel are caused by birefringence in the tooth associated with the probe light propagating perpendicular to the crystal axes of the enamel. These results indicated that polarization images in PS-OCT provide accurate information for detection of carious lesions.

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  • Investigating Or Analysing Materials By Optical Means (AREA)

Abstract

L'invention concerne un système d'imagerie optique sensible à la polarisation utilisé pour détecter des changements de polarisation dans les tissus dentaires et pour faciliter le diagnostic de maladies dentaires, telles que les caries. Pour mesurer le degré de dépolarisation, on illumine le tissu dentaire au moyen d'une lumière polarisée, puis on mesure l'état de polarisation de la lumière rétrodiffusée. L'état de polarisation de la lumière rétrodiffusée est analysé à l'aide de techniques d'imagerie polarimétrique optique. Une sonde dentaire portative à fibres optiques est utilisée in vivo pour diriger le faisceau incident vers le tissu dentaire et pour capter la lumière rétroréfléchie. Pour procéder à une caractérisation en profondeur du tissu dentaire, les analyses de l'état de polarisation peuvent être associées à des systèmes d'interférométrie à cohérence optique et de tomographie à cohérence optique permettant d'identifier les sites de dépolarisation de la subsurface présentant une déminéralisation de l'émail ou de l'os.
PCT/US2000/013878 1999-05-19 2000-05-19 Detection optique de maladies dentaires au moyen d'une lumiere polarisee Ceased WO2000069333A1 (fr)

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AU51476/00A AU5147600A (en) 1999-05-19 2000-05-19 Optical detection of dental disease using polarized light

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US31484899A 1999-05-19 1999-05-19
US09/314,848 1999-05-19

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DE102004026630B4 (de) * 2004-05-27 2007-05-03 Doctorseyes Gmbh Verfahren und Vorrichtung zur Makrofotografie
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CN106491082A (zh) * 2016-10-11 2017-03-15 明基电通有限公司 三维轮廓扫描器
CN108335324A (zh) * 2018-01-29 2018-07-27 清华大学 基于偏振瞬态成像的散射场景深度重建方法以及设备

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Cited By (20)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
USRE42641E1 (en) 1997-06-02 2011-08-23 Case Western Reserve University Depth-resolved spectroscopic optical coherence tomography
US6735463B2 (en) 1997-06-02 2004-05-11 Joseph A. Izatt Doppler flow imaging using optical coherence tomography
US7102756B2 (en) 1998-09-11 2006-09-05 University Hospitals Of Cleveland Interferometers for optical coherence tomography and reflectometry
US6657727B1 (en) 1998-09-11 2003-12-02 Joseph A. Izatt Interferometers for optical coherence domain reflectometry and optical coherence tomography using nonreciprocal optical elements
US7362444B2 (en) 1998-09-11 2008-04-22 Case Western Reserve University Interferometers for optical coherence domain reflectometry
US20110109914A1 (en) * 2001-01-22 2011-05-12 Roth Jonathan E Method and apparatus for polarization-sensitive optical coherence tomography
US7826059B2 (en) 2001-01-22 2010-11-02 Roth Jonathan E Method and apparatus for polarization-sensitive optical coherence tomography
WO2002075242A3 (fr) * 2001-01-22 2002-11-21 Jonathan E Roth Procede et appareil de tomographie par coherence optique sensible a la polarisation
US6775007B2 (en) 2001-01-29 2004-08-10 Joseph A. Izatt Frequency-encoded parallel OCT and associated systems and methods
EP1262751A3 (fr) * 2001-06-01 2005-01-26 Firma Ivoclar Vivadent AG Dispositif et procédé d'analyse de lumière
US7006126B2 (en) 2001-06-01 2006-02-28 Ivoclar Vivadent Ag Color analyzing apparatus with polarized light source
EP1262750A3 (fr) * 2001-06-01 2005-01-19 Firma Ivoclar Vivadent AG Dispositif de définition de la couleur
DE10126887B4 (de) * 2001-06-01 2004-08-12 Ivoclar Vivadent Ag Farbfestlegungsvorrichtung
DE10126887A1 (de) * 2001-06-01 2002-12-05 Ivoclar Vivadent Ag Farbfestlegungsvorrichtung
US7061622B2 (en) 2001-08-03 2006-06-13 Case Western Reserve University Aspects of basic OCT engine technologies for high speed optical coherence tomography and light source and other improvements in optical coherence tomography
DE102004026630B4 (de) * 2004-05-27 2007-05-03 Doctorseyes Gmbh Verfahren und Vorrichtung zur Makrofotografie
DE102005052294A1 (de) * 2005-10-26 2007-05-03 Jaruszewski, Lutz, Dr. Messvorrichtung und Verfahren zur Bestimmung des Aktivitätsstatus initialkariöser Schmelzläsionen
EP1970694A4 (fr) * 2005-12-07 2013-02-13 Topcon Corp Instrument de mesure d'image optique
CN106491082A (zh) * 2016-10-11 2017-03-15 明基电通有限公司 三维轮廓扫描器
CN108335324A (zh) * 2018-01-29 2018-07-27 清华大学 基于偏振瞬态成像的散射场景深度重建方法以及设备

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