Download - Introduction to Biomedical Optics
School of EngineeringDepartment of Biomedical Engineering
Fall 2014-2015EENG624 – Biomedical Optics
Instructor: Jad AYOUB
Chapters
1. Introduction to biomedical optics
2. Single scattering: Rayleigh theory and Mie theory
3. Monte Carlo modeling of photon transport
4. Convolution for broad-beam responses
5. Radiative transfer equation and diffusion theory
6. Hybrid model of Monte Carlo method and diffusion theory
7. Sensing of optical properties and spectroscopy
8. Ballistic imaging and microscopy
9. Optical coherence tomography
10.Mueller optical coherence tomography
11.Diffuse optical tomography
12.Photoacoustic tomography
13.Ultrasound-modulated optical tomography
Chapter 1 - Introduction
• Motivation for Optical Imaging
• General Behavior of Light in Biological Tissue
• Basic Physics of Light-Matter Interaction
Motivation for Optical Imaging
1. Optical photons provide nonionizing and safe radiation for medical applications.
2. Optical spectra -based on absorption, fluorescence, or Raman scattering- provide biochemical information because they are related to molecular conformation.
3. Optical absorption, in particular, reveals angiogenesis and hypermetabolism, both of which are hallmarks of cancer; the former is related to the concentration of hemoglobin and the latter to the oxygen saturation of hemoglobin. Therefore, optical absorption provides contrast for functional imaging.
4. Optical scattering spectra provide information about the size distribution of optical scatterers, such as cell nuclei.
5. Optical polarization provides information about structurally anisotropic tissue components, such as collagen and muscle fiber.
Motivation for Optical Imaging (cont’d)
6. Optical frequency shifts due to the optical Doppler effect provide information about blood flow.
7. Optical properties of targeted contrast agents provide contrast for the molecular imaging of
biomarkers.
8. Optical properties or bioluminescence of products from gene expression provide contrast for
the molecular imaging of gene activities.
9. Optical spectroscopy permits simultaneous detection of multiple contrast agents.
10. Optical transparency in the eye provides a unique opportunity for high-resolution imaging of
the retina.
Behavior of light in Biological Tissue
Optical properties of biological tissue
Basic properties
• n [–]: index of refraction; e.g., 1.37
• μa [cm–1]: absorption coefficient; e.g., 0.1
• μs [cm–1]: scattering coefficient; e.g., 100
• g [–]: scattering anisotropy, <cosθ>; e.g., 0.9
Derived properties
• μt [cm–1]: total interaction (extinction) coefficient, μa + μs
• lt [cm]: mean free path, 1/ μt; e.g., 0.1 mm
• μs’ [cm–1]: reduced scattering coefficient, μs(1 – g)
• μt’ [cm–1]: transport interaction coefficient, μa + μs’
• lt’ [cm]: transport mean free path, 1/ μt’; e.g., 1 mm
• μeff [cm–1]: effective attenuation coefficient, (3μa μt’)1/2
• δ [cm]: penetration depth, 1/(3μa μt’)1/2; e.g., 5 mm
Light- Matter Interaction
Beer’s Law
• −𝑑𝐼/𝐼
𝑑𝑥= 𝜇𝑡
• 𝐼 𝑥 = 𝐼 0 𝑒−𝜇𝑡𝑥 = 𝐼(0)𝑒−𝑥/𝑙𝑡
I : Ballistic intensity
x : Pathlength
𝜇𝑡: Total interaction (extinction) coefficient
Spectra of major Biological Absorbers
Absorption and its biological origins
• Absorption cross section: 𝜎𝑎• Number of density: Na
• Absorption coefficient: total cross-sectional area for absorption per unit volume:
𝜇𝑎 = 𝑁𝑎𝜎𝑎• Light attenuates as it propagates in an absorbing medium:
𝑑𝐼
𝐼= −𝜇𝑎𝑑𝑥
𝐼 𝑥 = 𝐼0𝑒−𝜇𝑎𝑥 : Beer’s law
• Transmittance: 𝑇 =𝐼(𝑥)
𝐼0: Probability of survival after propagation over 𝑥.
Absorption and its biological origins
• Origin of absorption:
oHemoglobin (Oxygenated & de-Oxygenated)
oMelanin
oWater
Melanin absorbs (UV) light stronglywater can be highly absorbing in some spectral regions
Scattering and its biological origins
• Scattering cross section: 𝜎𝑠• Number of density: Ns
• Scattering coefficient: total cross-sectional area for scattering per unit volume:
𝜇𝑠 = 𝑁𝑠𝜎𝑠• Light attenuates as it propagates in an Scattering medium:
𝑑𝐼
𝐼= −𝜇𝑠𝑑𝑥
𝐼 𝑥 = 𝐼0𝑒−𝜇𝑠𝑥 : Beer’s law
• Transmittance: 𝑇 =𝐼(s)
𝐼0= 𝑒−𝜇𝑠𝑥 : Probability of survival after propagation
over 𝑥.
Scattering and its biological origins
• extinction coefficient : 𝜇𝑡 = 𝜇𝑎+𝜇𝑠 (Total interaction coefficient)
• The reciprocal of 𝜇𝑡 is the mean free path between interaction events
Biological structures of various sizes for photon scattering
Exercise 1
• In a purely absorbing (non-scattering) medium with absorption coefficient 𝜇𝑎, what percentage of light is left after a lightbeampropagates a length of L?
Exercise 1
• In a purely absorbing (non-scattering) medium with absorption coefficient 𝜇𝑎, what percentage of light is left after a lightbeampropagates a length of L?
Exercise 2
• In a purely absorbing (non-scattering) medium with absorption coefficient 𝜇𝑎, Derive the average length of survival of a photon?
Exercise 2
• In a purely absorbing (non-scattering) medium with absorption coefficient 𝜇𝑎, Derive the average length of survival of a photon?
Exercise 3
• In a purely scattering (non-absorbing) medium with scattering coefficient 𝜇𝑠, what percentage of light has not been scattered after the original lightbeam propagates a length of L?
Exercise 3
• In a purely scattering (non-absorbing) medium with scattering coefficient 𝜇𝑠, what percentage of light has not been scattered after the original lightbeam propagates a length of L?
Exercise 4
• In a purely scattering (non-absorbing) medium with scattering coefficient 𝜇𝑠, Derive the average length of survival of a photon.
Exercise 4
• In a purely scattering (non-absorbing) medium with scattering coefficient 𝜇𝑠, Derive the average length of survival of a photon.
Exercise 5
• In a scattering medium with absorption coefficient 𝜇𝑎 and scattering coefficient 𝜇𝑠 , what percentage of light has survived scattering and absorption after the original lightbeam propagates a length of L? Of the percentage that has been absorbed and scattered, what is the percentage that has been absorbed?
Oxygen Saturation and Concentration
• Estimating concentration by absorption coefficients (@ 𝜆1 ≠ 𝜆2):
• 𝜆1 , 𝜆2 : the two wavelengths
• 𝜀𝑜𝑥 , 𝜀𝑑𝑒: Molar extinction coefficients of oxy- and deoxyhemoglobin
• 𝐶𝑜𝑥 , 𝐶𝑑𝑒: Molar concentrations of oxy- and deoxyhemoglobin.
Oxygen Saturation and Concentration
• Once 𝐶𝑜𝑥 and 𝐶𝑑𝑒 are obtained, the oxygen saturation (𝑆𝑂2) and the total concentration (𝐶𝐻𝐵) of hemoglobin can be computed as follows:
• This principle provides the basis for pulse oximetry and functional imaging. Angiogenesis can increase 𝐶𝐻𝐵, whereas tumor hypermetabolism can decrease 𝑆𝑂2.
Application: NIRS (Near IR spectroscopy)