01 Biomedical Instrumentation - Origin of Bioelectric Potentials
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Transcript of 01 Biomedical Instrumentation - Origin of Bioelectric Potentials
Biomedical Instrumentation -
Origin of bioelectric potentials
prof.dr.sc. Ratko Magjarević
University of ZagrebFaculty of Electrical Engineering and
Computing
Outline
• Introduction
– Definition of BME
– Achievements of Biomedical Engineering in 20th Century
– Challenges of Biomedical Engineering for 21th Century
– Why to study Biomedical Engineering?
• Origin of bioelectric signals
2
Human physiology
• Science on vital processes and functions inliving organisms
• BME students have special interest in:
– Electrophysiology
– Control mechanisms
“A man is a machine, extremely complex, but
still a machine” (Arthur Vander)
3
Electrophysiology
• Study of electric properties of biological cellsand organs
• Includs measurement of voltage changes andcurrents from cell level to organ level
• In neuroscience, potentials of nerve cells andaction potentials are measured
4
Types of electrophysiological
measurements
• Electrocardiography (abb. ECG or EKG)- a standard noninvasive procedure for recording electrical potentials of the heart. The record (electrocardiogram), consists of waves that relate to the electrical activity of the heart during each beat. Results - printed on paper or displayed on monitor.
5
Types of electrophysiological
measurements
• Electroencephalography (EEG)- a standard noninvasive procedure for recording electrical activity of the brain. The record (electroencephalogram), consists of curves that relate to the spontaneous electrical activity of millions ofneural cells of the brain. The recording lasts for 20- 40 min and is printed on paper or displayed on monitor.
6
Types of electrophysiological
measurements
• Electromyography (EMG)-
• recording the electrical activity produced by skeletal muscles.
• Electrooculography (EOG) - measuring the resting potential of the retina. The resulting signal is called the electrooculogram.
• Other methods: Electroretinography,
Audiology, Electrogastrography ...
7
Human body structure
• Chemical elements
• Cells
• Tissue – group of similar cells
• Organ – group of similar tissues
• System – functional complex made ofdifferent organs
• Organism – functional complex of 11 systems
8
Human body composition
- the structural level
• Chemical level
• Cellular level
• Tissue level
• Organ level
• System level
• The level of the organism
9
Human body chemical composition
• Most represented elements (approx. 99,3%):
– Hydrogen (H) 63%
– Oxygen (O) 26%
– Carbon (C) 9%
– Nitrogen (N) 1%
10
Human body chemical composition
• Minerals (approx 0,7%):
– Calcium (Ca)
– Phosphorus (P)
– Potassium (K)
– Sulphur (S)
– Sodium (Na)
– Chlorine (Cl)
– Magnesium (Mg)
11
Human body chemical composition
• Other elements (<0,01%):– Iron (Fe)– Iodine (I)– Copper (Cu)– Zinc (Zn) – Manganese (Mn) – Cobalt (Co) – Chromium (Cr) – Selenium (Se) – Molybdenum (Mo) – Fluorine (F) – Tin (Sn) – Silicon (Si) – Vanadium (V)
12
Human organism consists of
Fluids
(approx. 2/3 of the weight)
+
Tissues
(groups of similar cells)
13
Liquids
• Intracellular fluid ( approx. 40%)
• Extracellular fluid (approx. 20%)– Interstitial fluid (approx. 16%)
– Plasma (approx. 4%)
• The remainder (6-10%) consists of:– Blood
– Lymphatic fluid
– Urine
– Cerebral spinal fluid
14
Tissues
NERVOUS
(Neural)
MUSCLE
(Muscular)
CONNECTIVE EPITHELIAL
1. NERVOUS(Neural)
1. SKELETAL(Voluntary)
1. FILAMENTARY(Fibrous)
1. VESSELS(Vascular)
2. GLIA CELLS(Cells for excitacion
of brainmetabolism)
2. SMOOTH(Involuntary)
2. FAT (Adipose)
2. GLAND(Gladular)
3. CARDIAC(Involuntary)
3. CARTILAGINOUS 3. SKIN
4. BONES(Osseous)
4. HAIR(Cilia)
15
Cell
• Human organism consists of approx. 75·1018
cells (75.000.000.000.000.000.000)
• Cell diameter ranges from 0,2 - 120 µm
• Most cells range from 10 - 20 µm in diameter
• Organisms of different sizes (man or elephant) consist of cells similar in dimension, only thenumber of cells is different
16
Cell structure
Subcellular components
(1) nucleolus
(2) cell nucleus
(3) ribosome
(4) vesicles
(5) rough endoplasmic reticulum(ER)
(6) Golgi
(7) Cytoskeleton
(8) smooth endoplasmic reticulum
(9) mitochondria
(10) vacuole
(11) cytoplasm
(12) lizosom
(13) centrioles
17
Cell membrane
• Cell membrane is semipermeable lipid bilayer made of lipids and proteins that separates the intracellular part from the extracellular environment
• Thickness of 10 nm
• Semipermeable - the pore width 8 nm
• Dielectric constant ε = 5, spec. capacity C = 0.5 to 1 μF/cm2
• Transit of substances (in and out of cells) is regulated by– Diffusion (from regions of higher concentration to regions of lower concentration)
– Osmosis (diffusion of water through a semipermeable membrane)
– Active transmission (from region of lower concentration to regions of higher concentration, requires energy)
• State of the membrane is determined by two main factors:– Concentration gradient (diffusion coefficient, D)
– Electric field (E)
18
Concentration in the cell and
out of the cell
* mM/l, millimol per liter
Phospates
Amnino acids
Glucose
19
Cell membrane
• Potassium ions (K+) exit the cell easily, while A- is hard to come out of thecell
• Na+ is hard to enter, whereas Cl- enters the cell easily • Na-K pump ejects Na+ more efficiently than injecting K+ • Therefore, outside the cell there is an excess of positive charge and the
inside of the cell is negatively charged
a) Cell polarization b) part of the membane c) structure of the membrane
Extracellularspace
Intracellularspace
20
Diffusion through semipermeable
membrane - the passive process
x
cDS
t
m ixi
d
d
d
d⋅⋅=• Fick’s law
mi = amount of (a particular) substance i [mol] t = time [s]S = membrane surface [m2]D = diffusion coefficient [m2/s] dcix / dx = concentration gradient [mol/m3] of a particular substance i at the possition x
• diffusive flux goes from regions of higher concentration to regions of lower concentration, and it is proportional to the concentration gradient (in space).
• K+ ions can easily leave the cell, creating an excess positive charge and the potential difference occurs - diffusion takes place until the electric field is established and it stops the process of diffusion
21
Sodium - Potassium Pump –
an active process
• Na+ + Y-complex= NaY molecule + Na-pump = Out Na+ + X• K+ + X-complex = KX molecule + K-pump = In K+
•For each inserted K + ion, 2-5 Na + ions are ejected
•Na-K pump requires energy:
ATP = ADP + energy
ATP - adenosine triphosphate, ADP - adenosine diphosphate22
Resting potential
The resting potential of a cell -
Nernst equation
∆u = potential difference [V]
R = universal gas constant = 8,314 J/molK
T = absolute temperature (0K = -273 °C)
n = valence of chemical elements whose concentration is considered, potasiuminthis case
cki , cko = concentration of ions inside and outside the cells
F = Faraday constant = 96,5 C/mol
E = electric field [V/m]]
cm
kV[ 85
[nm] 10
[mV] 85
membrane on the field Electric
[mol/l]140 ,[mol/l] 5 ,C][ 37
mV 85
[mV] log 5.61
ln2
1
==∆
=
==°=
−=∆
=∆
⋅
⋅=∆
d
uE
ccT
u
c
cu
c
c
Fn
TRu
KiKo
Ki
Ko
k
k
23
Resting potential
Bioelectric potentials are a result of electrochemicalactivity of excitable cells (in neuros, muscular orglandular system)
The resting potential of a cell – steady difference inelectric potentials between internal and externalenvironment of the cell.
Typical values of resting potentials are in range of -50 mVto -100 mV (reference point out of the cell).
24
Action potential
• Stimulus:
– Mechanical
– Chemical
– Electrical
• Sudden increases of membrane conductance for Na + ions (1000 times more) - change in polarity of the voltage - depolarization
threshold
conductivity
Depolarization
Action potential, showing depolarisation andrepolarisation b) Changes in conductivity forsodium and potassium during the action potential
Repolarization
Stimuli
25
Action potential
• After commencement of the action potential , the process can not be stopped by any subsequent stimulus - as long as this state lasts we are talking about the absolute refractory period t
o
• When the process starts to calm down and return power to the value at rest, it is possible to re-trigger action potentials using more intense stimulus, even though the voltage has not reached the value at rest - the time when it is possible to re-create the action potentials with a greater intensity of stimulus is called the relative refractory time, t
r
threshold
stimulus30
-85Restingpotential
a) Action potential b) Two consecutive action potentials, caused by stimuli S1 and S2. Note that themagnitude of S2 is larger than magnitude of S1
S1
S2
26
Action potential
• The course:
– The stimulus reaches the threshold
– Increasing membrane permeability for Na + ions
– After that, permeability for K + increases and Na + ions permeability decrease
– Reducing permeability for K + ions
– Active ejection of Na + and injection of K + ions
27
Action potential
• Excitable cells have the ability to conduct action potentials whenadequatly stimulated.
• An adequate stimulus causes depolarisation of the membrane largeenough to reach and exceed the stimulation threshold of the membrane.
• Adequate excitation causes an action potential, which follows the all –or-none rule. The action potential travals along the membrane at constantvelocity and without attenuation.
• At rest, the cell is said to be polarized.
• After the cell is excited, the potenetial is decreasing – depolarisation ofthe cell membrane.
• Returning of the cell potential to the resting value is called repolarisation.
• After repolarisation, for a short period of time, the cell potential isincreased which is called hyperpolarisation. During that period, a stimulushas to be of larger magnitude in order to excite a cell.
28
Cell membrane model
• Hodgkin and Huxley – Nobel prize, 1963Resting potential u
Intracellular medium
Extracellular medium (liquid)
Diagram of network equivalent circuit of a cell membrane showing voltagesources of main ions Ei, membrane conductances gi and membrane capacitance C.
29
Nerve cell
Cell body (soma)
Dendrites
Axon
Nucleus
Synapses
Intercommunicating links between neurons (neuro-neuro junctions) are calledsynapses.
30
Transfer of stimulus - Synapse
• Stimulus stimulatesneurotransmitter secretion in the synaptic cleft and stimulates (or not) the next nerve cell
• Neurotransmitters: – Acetylcholine
– Monoamines
– Amino acids
– Peptides
• Synapses can be:– excitation
– inhibitory
Action potential
presynapsis
Synapticgap
Neurotransmitterrelease
postsynapsis
31
Synapse activity
Changes in resting potential caused by activity at an excitatory and an inhibitorysynapse
Stimuli
Stimulation threshold
depolarisation
hyperpolarisationExcitatorysynapsis Inhibitory synapsis
32
Temporal and spatial summation
Stimulationthreshold
Temporalsumation
Spacial sumation
Stimuli
33
Types of synaptic connections
• Neuron – neuron junctions
• Neuromuscular junctions – communicationlinks between neurons and muscle fibers. These are small regions of the muscle fiber, called neuromuscular plates.
34
Types of nerve fiber
• Myelinated fibers– Axon is insulated by a seath of myelin (lipoprotein) – Myelin seath interrupted every 1-2 mm nodes of Ranvier– Sodium ion chanells distributed unequally, more at nodes
of Ranvier– Myelization reduces leakage currents and improves
transmission properties (cable like behaviour)– faster propagation of action potentials
• Unmyelinated– Equal distribution of sodium and potassium channels– Leackage current sourses more expressed– Slower propagation along the axon (cable)
35
Propagation of stimuli in unmyelinedand in myelined nerve fibers
Stimulus
Potential differencemeasured along the fibre
Schwan cell
Node of Ranviermyelin
36
Human Sences
• Enable tracking of happenings in the outside world
• Convert external information in forms suitable for processing in the nervous system
37
Types od sences according to
types of stimulus
• Mechanoreceptors– touch, pressure, hearing
• Thermoreceptors– hot, cold
• Chemoreceptors– smell, taste (salty, sweet, sour and bitter), reaction to O2
and CO2
• Photoreceptors– vision
• Nocireceptors– pain, damage
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Sences
• Sences that react to touch and pressure: • The free end - without a myelin sheath • Nerve ending in a cocoon - Pacinij corpuscles, Krause end bulb,
Markel corpuscle, Meissner corpuscles, Ruffine corpuscle39
Receptor potentials
• Sensory cells have a high threshold of excitability
• Stimulus does not produce an action potential - the potential value changes - receptor or generator potential
• Change in resting potential due to intensity of the stimulus– linear
– logarithmic
40
Receptor potentials
a) Tactile receptor excited by the force Fb) Receptor potential Ur and frequency f of action potentials against
relative intensity of excitation; I0 – thresholf of stimulation c) Intensity of excitation I, receptor potential Ur and action potential
Uak generation - frequency response
Node of Ranvier
Stimuli
41
Accommodation, habituation
• Receptor potential is reduced when stimulation lasts a longer period of time with the same intensity
– most expressed for the sence of touch
– negligible for the sense of pain
42
Voltage - frequency conversion
• Voltage frequency conversion occurs at the firstnode of Ranvier on the axon
• Pulse frequency is linearly proportional to the receptor potential
• The relationship between pulse frequency and intensity of stimulation:
– n <1 - sence compression (eg, logarithmic curve), present in vision and hearing
– n = 1 - a linear relationship
( )n
0k IIf −=
43
Sences with nonlinear (logarithmic) relationship
between stimulus intensity and sensory reception
• Nonlinear (logarithmic) relationship is necessary wheneverthere are large differences in the intensity of stimuli
• E.g., the ratio between whisper sound intensity and sound of a jet airplane, or between moonligth and day sunlight is 1:106
• In a logarithmic relations, the frequency of generated action potentials changes in ratio 1:13,8
• The highest frequency of action potentials in nerve fibers iscorresponding to the reciprocal value of absolute refractory time and is approximately 1000 Hz,
• Most receptors have highest frequency in order ofmagnitude of hundred Hertz
44
• Sence S is proportional to the relative intensity change I (Weber-Fechner Low):
0
0
ln
0 za ln ,01
ln
01
I
IkS
SCICSk
I
dSkI
dI
I
dIkdS
I
IkS
=
=−==+−
=−
=→∆
=∆
Sences with nonlinear (logarithmic) relationship
between sense and stimulus intensity
45
Sence of hot and cold
46
Sence of sight
• The sence in which we receive most information from the outside world– cerebral cortex provides the greatest surface area
for receiving, processing and synthesis of theimage
• Sences are located in the eyes(photoreceptors) – sensitive to light intensity (stick cells, 125·106)
– sensitive to color (cone cells, 6·106) • Red, green, blue
47
Sence of sight
Cross section of the eye and the cross section of retina
48
Sence of sight
• A sharp image comes on the central part of the retina where there are mostly cones -yellow spot (fovea centralis)
• At the point where ganglion cell axons (up to106) exit, there are no photoreceptors and theimage that comes on that part of the retina is not visible - blind spot
49
Cones and sticks arrangement along
the retina
• Sticks are deployed across the retina• Cones concentration is highest in the ± 4 ° area around the
Fovea
Sticks Cones
FoveaBlindspot
50
Information reduction
• Reducing the useless information load of thevision center
• Reduction is allowed by the horizontal and amacrine cells - predominantly contain inhibitory synapses
• Enable good observation of the contour (outline) of an object, rather than the contents inside the contour, which often (except data on the color and intensity of light) do not contain otherimportant information
51
Literature
• A. Šantić: Biomedicinska elektronika, Školska knjiga, Zagreb; 1995
• John G. Webster: Medical Instrumentation
Chapter 4, The origin of biopotentials
• R.S. Kandpur: Biomedical Instrumentation, Chapters 1.1-1.3, 2.1
52