Patent Application
20220249865
The present disclosure relates to a pulse application method and a pulse application device.
Coagulation treatment in which collagen fibers are heated to coagulate the collagen fibers by application of laser light to skin has been performed as skin treatment (for example, “Current Laser Resurfacing Technologies”: A Review that Delves Beneath the Surface, Jason Preissig, Kristy Hamilton, Ramsey Markus, Seminars in Plastic Surgery, Vol. 26, No. 3, 2012, PP. 109-116).
In some embodiments, A pulse application method includes: setting a wavelength of light within a range in which a temperature rise width of collagen fibers in living tissue when the light is applied to the living tissue is larger than a temperature rise width of water containing cells that are contained in the living tissue and that are present around the collagen fibers; and applying a pulse of light with the set wavelength to the living tissue to heat the living tissue.
In some embodiments, a pulse application device includes: a pulse laser device configured to emit a pulse of light; and a controller configured to set a wavelength of the light within a range in which a temperature rise width of collagen fibers in living tissue when the light is applied to the living tissue is larger than a temperature rise width of water containing fibroblast that are contained in the living tissue and that are present around the collagen fibers, and cause the pulse laser device to apply the pulse of light to the living tissue with the set wavelength to heat the living tissue.
The above and other features, advantages and technical and industrial significance of this disclosure will be better understood by reading the following detailed description of presently preferred embodiments of the disclosure, when considered in connection with the accompanying drawings.
An exemplary embodiment of the disclosure and modifications thereof will be disclosed below. Configurations of the embodiment and the modification presented below and the functions and results (effects) brought by the configurations are an example. The embodiment can be realized by a configuration other than the configurations disclosed by the embodiment and the modifications below. According to the disclosure, it is possible to obtain at least one of various effects (including derivative effects) obtained by the configurations described below.
Configuration of Pulse Application Device
The pulse laser device 10 is capable of emitting a pulse of infrared laser light. The pulse of laser light that is emitted by the pulse laser device 10 is transmitted to the optical head 20 via the optical fiber 30 and is applied from the optical head 20 to skin S. The optical head 20 disperses and collimates or focuses the pulse of laser light and applies the pulse of laser light to the skin S. The skin S is heated and/or stimulated by the applied pulse of laser light. The optical head 20 is moved manually or a robot arm, or the like, making it possible to apply the pulse of laser light to a desired spot on the skin S. The control device 40 is able to set or change a specification, such as an intensity of a pulse of laser light that is emitted from the pulse laser device 10, a pulse application time period (a pulse ON period or a pulse width) of the laser light and a pulse non-application time period (pulse OFF period) of the laser light. The pulse laser device 10 may include a fiber laser device or a semiconductor laser device. The skin S is an example of living tissue.
The sensor 50 detects a thermal denaturation state of collagen fibers that are contained in the skin S. The thermal denaturation state of collagen fibers will be described, exemplifying a cornea. A cornea is mainly composed of collagen and, because collagen fibers are aligned in the cornea, the cornea has high transparency in the state of not thermally denaturing. When a structure change occurs in collagen in the cornea due to thermal denaturation, the structurally changed part becomes the center of scattering and the cornea becomes cloudy in a visible light region. Based on the same principle, it is possible to detect a thermal denaturation state of the skin S by measuring a scattering state by the optical sensor 50, for example, measuring back scattering attenuation of irradiation light. In this case, the sensor 50 is a non-contact sensor. When the skin S thermally denatures, the hardness of the skin S increases. Thus, measurement of hardness by the mechanical sensor 50, such as a hardness sensor, enables detection of a thermal denaturation state of the skin. In this case, the sensor 50 is a contact sensor. It is possible to detect a thermal denaturation state of collagen molecules not only in a cornea but also in other tissue. The control device 40 is able to end application of pulses at a time when the sensor 50 detects a given thermal denaturation state of collagen fibers. The sensor 50 is an example a detector.
Tissue of Skin (Living Body)
Setting of Wavelength of Laser Light
Based on such nature, in the present embodiment, the wavelength of laser light to be applied to the skin S, that is, the wavelength of laser light that the pulse laser device 10 emits is set within a range in which the absorption coefficient of collagen molecules is larger than the absorption coefficient of water, that is, is set longer than 1480 [nm]. It can be argued that the range in which the wavelength is longer than 1480 [nm] is a range in which collagen fibers (collagen fiber bundles) are heated more easily than water.
As described above, in the range in which the wavelength is longer than 1600 [nm], the absorption coefficient of collagen molecules decreases as the wavelength becomes longer and this means that an optical energy absorption efficiency of collagen molecules decreases depending on application of laser light whose wavelength is longer than 1600 [nm]. Thus, in the present embodiment, the wavelength of laser light that is applied to the skin S, that is, the wavelength of laser light that the pulse laser device 10 emits is set equal to or under 1600 [nm].
From such consideration, in the present embodiment, the wavelength of laser light that is applied to the skin S, that is, the wavelength of laser light that the pulse laser device 10 emits is set longer than 1480 [nm] and equal to or under 1600 [nm].
Setting of Pulse Application Time Period and Pulse Non-Application Time Period
As illustrated in
The inventors focused on the aspect that the temperature of collagen fibers rises during the pulse application time period Ton and calculated a pulse application time period Ton makes it possible to further increase the absorption coefficient ratio.
As illustrated in
On the other hand, as illustrated in
The inventors focused on the aspect that the temperature of water decreases in the pulse non-application time period Toff and calculates the pulse non-application time period Toff that makes it possible to selectively heat collagen fibers while inhibiting the temperature of water from rising.
It was proved that, as illustrated in
It can be understood that, as illustrated in
It is preferable that the pulse non-application time period Toff be set according to a thermal relaxation time period of collagen fibers. The thermal relaxation time period of collagen fibers may be defined as a time period from the end of the pulse application time period Ton immediately before the pulse non-application time period Toff until a time when the temperature of collagen fibers decreases to a temperature obtained by adding a temperature width (Δtc/e) obtained by dividing a temperature rise width of collagen fibers in the pulse application time period Ton by a bottom of a natural logarithm to the temperature at the start of the pulse application time period Ton. Here, Δtc is the temperature rise width of collagen fibers.
The pulse non-application time period Toff can be set longer than the thermal relaxation time period of collagen fibers. In an example, the pulse non-application time period Toff may be set at a value obtained by multiplying the thermal relaxation time period by a coefficient larger than 1 (for example, 1.1, or the like). In this case, the temperature of water at the end of the pulse non-application time period Toff tends to be equal to or lower than the temperature of water at the start of the pulse application time period Ton immediately before the pulse non-application time period Toff. This makes it possible to assuredly inhibit the temperature of water from rising.
The pulse non-application time period Toff can be set equal to the thermal relaxation time period of collagen fibers. In this case, the temperature of water at the end of the pulse non-application time period Toff is equal the temperature of water at the start of the pulse application time period Ton immediately previous to the pulse non-application time period Toff. It is possible also in this case to inhibit the temperature of water from rising.
The pulse non-application time period Toff can be set shorter than the thermal relaxation time period of collagen fibers. In an example, the pulse non-application time period Toff may be set at a value obtained by multiplying the thermal relaxation time period by a coefficient (for example, 0.9, or the like) larger than 0 and smaller than 1. In this case, the temperature of water at the end of the pulse non-application time period Toff is higher than the temperature of water at the start of the pulse application time period Ton immediately before the pulse non-application time period Toff. In other words, it is higher than the temperature of water at the end of the pulse non-application time period Toff presented in
Furthermore, regardless of the length of the pulse non-application time period Toff, the highest temperature of water in the pulse application time period Ton is set, for example, equal to or smaller than a temperature that does not damage the skin S. The temperature that does not damage the skin S in this case is an example of a second temperature. The second temperature is a threshold temperature that is set according to the temperature of water at the end of the pulse application time period Ton.
Normally, the higher the temperature is, the shorter the time in which protein thermally denatures is and, the lower the temperature is, the longer the time in which protein thermally denatures is. The protein of which a living organism consists causes an irreversible thermal denaturation at approximately 60° C. In some cases, although it varies depending on the site or internal organ and varies depending on the heating time, thermal damage may occur in living tissue even at approximately 45° C. when the heating time is relatively long. It is possible to acquire a threshold temperature corresponding to a site of irradiation, an irradiation environment, an irradiation condition, etc., experimentally in advance (refer to Literature 2: Minoru Obara, Tsunenori Arai, Katsumi Midorikawa. Applied Laser Engineering. Corona Publishing Co., Ltd., 1998.)
The thermal relaxation time period varies depending on the water content of the skin S, arrangement of collagen fibers (fiber bundle of collagen fibers) in the skin S, the intensity of laser light, the pulse application time period Ton, etc. Thus, the thermal relaxation time period and the pulse non-application time period Toff may be set variably according to the water content of the skin S, arrangement of collagen fibers in the skin S, the intensity of laser light, the pulse application time period Ton, etc.
The pulse application time period Ton, the pulse non-application time period Toff and the energy (intensity) applied in the pulse application time period Ton may be the same among multiple pulses or may differ per pulse. For example, the control device 40 may change at least one of the pulse application time period Ton, the pulse non-application time period Toff, and the energy according to the denaturation caused by heating of collagen fibers.
During the pulse application time period Ton, the pulse of laser light may be applied intermittently like a burst waveform. The time of intermittence in this case is, for example, sufficiently shorter than the thermal relaxation time period.
In order to obtain the effect of a single pulse, the wavelength of laser light and the pulse application time period Ton are set such that the collagen molecules in collagen fibers thermally denature. In order to obtain the effect of multiple pulses, the wavelength of laser light, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that collagen molecules in collagen fibers thermally denature.
Locally and selectively heating living tissue by repetitive application of pulses of laser is a method of, when the absorption coefficient of tissue to be heated selectively is larger than the absorption coefficient of surrounding tissue, selectively heating tissue with a large absorption coefficient by adjusting the pulse width (the pulse application time period Ton) and the pulse interval (the pulse non-application time period Toff). This method is referred to as selective photothermolysis (refer to Literature 3: Selective photothermolysis: precise microsurgery by selective absorption of pulsed radiation, R R Anderson, J A Parrish, Science, Vol. 220, Issue 4596, PP. 524-527, 1983).
Specifically, adjustments of the pulse width and the pulse interval are made in consideration of heat conduction to the surroundings in the pulse interval. The state of heat conduction to the surroundings is determined by the heat conductivity and the shape of a heat generating part. In order to simply argue the issue of unsteady heat conduction, a feature heat conduction (thermal relaxation constant) is defined and used. For selective photothermolysis, the pulse width is set sufficiently shorter than the feature heat conduction time and the pulse interval is set sufficiently longer than the feature heat conduction time (Literature 2).
Selective photothermolysis does not give a heat generation contrast equal to or more than the absorption ratio between a living tissue part whose light absorption is large and the surrounding living tissue whose light absorption is small (in other words, the heat generation ratio depending on laser application) and the absorption ratio gives an upper limit of the heat generation ratio. On the contrary, when a sequential laser is applied for a long time, because the heat conduction leads to uniform heating, local and selective heating cannot be realized.
Thermal denaturation of collagen molecules includes irreversible thermal denaturation and reversible thermal denaturation. Irreversible thermal denaturation causes coagulation of collagen molecules and is used for treatment of cancers, coagulation of retina, hemostasis, etc. Reversible thermal denaturation of collagen molecules is used to weld a blood vessel, the small intestine, skin, etc.
Collagen molecules form three-dimensional spiral structure chains; however, the hydrogen bonds that bind the spiral structure chains are disconnected with an increase in temperature and, when overheated, the collage molecules are dispersed and shrink. This state is irreversible thermal denaturation. In the case of denaturation with a small ratio of disconnection of bonds, a return to the original structure is made in some cases and this transient thermal denaturation is referred to as reversible thermal denaturation. Collagen molecules are classified into a few tens of types according to the types and shapes of amino acid contained and the site of presence in living tissue differs. In the present embodiment, I or III collagen serving as main components of skin, skin loss repair, bone, etc., is main referred to. The physical properties of collagen molecules differ also depending on animal species and thermal properties differ depending on the environment in which the living organism lives (refer to Literature 4: On a Relationship Between the Arrhenius Parameters from Thermal Damage Studies, Neil T. Wright, Journal of Biomechanical Engineering, Vol. 125, No. 2, PP. 300-304, 2003). In the present embodiment, thermal properties of collagen molecules of mammals including human beings living on land are mainly referred to.
Thermal denaturation of collagen molecules is one type a chemical reaction process and is described according to Arrhenius theory (Equation (1), Arrhenius equation) describing a chemical reaction (refer to Literature 5: Finite element analysis of temperature controlled coagulation in laser irradiated tissue, T. N. Glenn, S. Rastegar, S. L. Jacques, IEEE Transactions on Biomedical Engineering, Vol. 43, No. 1, PP 79-87, January 1996, Eq(3)).
where Ω: stored heat denaturation amount, A: frequency factor [1/s], Δt: heating time [s], Ea: activation energy [J/mol], R: gas constant [J/mol·K](≈8.314), and T: temperature [K]. The stored heat denaturation amount is a guide of denaturation and, in general, at approximately 1, it is determined that it is thermal denaturation.
From Equation (1), when the heating time is constant, the stored heat denaturation amount is proportional to the time. The power of an index function is a negative number and the frequency factor and the stored heat denaturation amount are constants that are determined by the substance and thus, the higher the temperature is, the larger the value of the exponential function is. Accordingly, the thermal denaturation depends on the heating time and the holding time.
The fact that the stored heat denaturation amount is a guide of a denaturation amount and does not provide a precise threshold is taken as the reason why the stored heat denaturation amount based on Arrhenius theory is not used in general. Furthermore, the frequency factor and the activation energy vary depending on the substance (protein). As described above, while Arrhenius theory can give a theoretical support on living organism protein coagulation, standing on precise Arrhenius theory has less meaning in a practical broad argument. Thus, in general, a determination is made based on a thermal denaturation temperature serving as a guide (refer to Literature 6: Photophysical processes in recent medical laser developments: A review, Jean-Luc Boulnois, Lasers in Medical Science, January 1986, Volume 1, Issue 1, PP. 47-66).
A practical heat application time in a spot in living organism treatment is short because it is a local action particularly in an operation treatment device and does not exceed, for example, one second. In a burn that is a typical living organism thermal damage, heating does not continue because of a living biology reaction response and, typically, it is approximately 50 ms. As described above, as a result of limitation of on the heating time in treatment, a temperature that gives a sufficient accumulated thermal denaturation amount is determined roughly.
As described above, it is difficult to precisely obtain a temperature and a heating time that are necessary to obtain irreversible thermal denaturation of living tissue and a guide value of a temperature enabling irreversible thermal denaturation is used practically (refer to Literature 6). In the present embodiment, a generally-used guide value of a temperature enabling irreversible thermal denaturation is used as a threshold temperature. When a thermal denaturation threshold temperature is exceeded, protein thermally denatures and, when a reversible thermal denaturation threshold temperature is exceeded, protein reversibly thermally denatures.
Fibroblast are cells that generate collagen molecules and thus it is preferable that the temperature of fibroblast, that is, the temperature of water be a temperature at which fibroblast are not damaged, that is, a temperature causing no thermal denaturation. As for fibroblast, it has been proved that activities are activated by heating fibroblast to an extent where the fibroblast are not damaged to cause the fibroblast to reversibly thermally denature.
When protein in fibroblast cause irreversible thermal denaturation, vital activity stops and the cells necrose (thermal damage or irreversible thermal damage). On the other hand, when reversible thermal denaturation of protein or significantly little and local irreversible denaturation of protein occurs, in some cases, homeostasis causes restoration outcome (activation) of the fibroblast (reversible damage). Fibroblast may go into necrosis because cytoplasm goes out of the cells via pores that are opened due to thermal damage of the surrounding phospholipid bilayer and the surrounding body fluid flows into the cells via the cell membrane and causes the cells to swell and the cells rupture. In thermal coagulation treatment, formation of pores in the cell membrane and thermal denaturation of protein are caused and thresholds thereof remain a subject of dispute. Thermal denaturation of protein tends to be used for general modeling.
Selective heating can be executed under a condition that causes thermal transpiration on the surface of living tissue. Thermal transpiration of living tissue occurs at the moment when the temperature of moisture in living tissue reaches 100° C. locally and boils. When water in the liquid phase turns into steam, the volume expands approximately thousandfold, the cell membrane is torn and the tissue disappears. In order to cause this to occur successively, a condition that sequentially supplies latent heat that is lost due to boiling can be set (refer to Literature 2).
In order to obtain an effect of a single pulse, the wavelength of laser light and the pulse application time period Ton are set such that fibroblast are not thermally damaged or are reversibly thermally damaged. In order to obtain the effect of multiple pulses, the wavelength of laser light, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that fibroblast are not thermally damaged or are reversibly thermally damaged.
In the present embodiment, the longer the pulse application time period Ton is, the higher the temperatures of collagen fibers and water (fibroblast) increase and, the longer the pulse non-application time period Toff is, the lower the temperatures of collagen fibers and water (fibroblast) are. The difference of the temperature of collagen fibers after the end of the pulse non-application time period Toff from the temperature of collagen fibers at the start of the pulse application time period Ton and the difference of the temperature of water (fibroblast) at the end of the pulse non-application time period Toff from the temperature of water (fibroblast) at the start of the pulse application time period Ton is adjustable by the wavelength, the pulse application time period Ton and the pulse non-application time period Toff. The number of times the pulse application time period Ton is repeated (also simply referred to as a repetition number-of-times below) can be set based on the defenses in temperature thereof. For example, in the situation where each of the temperatures increases in each set of the pulse application time period Ton and the pulse non-application time period Toff, the larger the difference in temperature is, the smaller the repetition number-of-times until the time when each of the temperatures reaches a given temperature is and, the smaller the difference in temperature is, the larger the repetition number-of-times until the time when each of the temperatures reaches the given temperature is. The wavelength of laser light, the pulse application time period Ton, the pulse non-application time period Toff, and the repetition number-of-times can be set in consideration of an environmental condition, such as the ambient temperature or the body temperature. Note that the lengths of the pulse application time period Ton and the pulse non-application time period Toff need not be set the same (at constant values) with respect to a plurality of sets of pulse application and the lengths may be switched when it comes close to a given temperature or may be changed per pulse.
In the pulse application device 1 illustrated in
For example, when high speed scanning of laser light is made with the Galvano scanner in the space optical system, laser light is applied to a certain point on the skin S for a period corresponding to a scanning speed. In this case, even when the laser light that is emitted by the pulse laser device 10 is a continuous wave, it is possible to apply the laser light to the skin S in a manner of pulses. For example, the trajectory of laser light by scanning may be in a shape of a ring. Accordingly, laser light is applied in a manner of pulses repeatedly to sequential points on the skin S and, even when laser light is a continuous wave, it is possible to control heat input to the skin S over time.
A control mechanism for controlling a beam profile of laser light may be further added to the pulse application device 1. As such a control mechanism, a mechanism that includes a special optical fiber and that generates a beam that is a combination of a beam of a single-peak-type profile and a beam of a ring-type profile is known. As another control mechanism, a mechanism including a spatial light modulator (SLM) is known. The SLM is, for example, a space phase modulation device that consists of pixels of a phase modulation device that are a plurality of micro-optical operation devices that are arrayed one-dimensionally or two-dimensionally and that controls the beam profile of input laser light by electrically controlling the phase of each of the pixels.
Furthermore, as another control mechanism, a mechanisms including a DOE (diffractive optical element) is known. The DOE is a diffractive optical element configured by integrating a plurality of diffraction gratings with different periods. The DOE is capable of forming a beam shape by deflecting input laser light to a direction of an effect of each diffraction grating or superimposing the laser light. For example, the DOE is capable of forming the input single-peak-type beam into a line beam or a ring beam.
The pulse application device 1 includes the single pulse laser device 10; however, the pulse application device 1 may include a plurality of the pulse laser devices 10. When a plurality of the pulse laser devices 10 are included, the wavelengths of laser light to be emitted may be all the same or may differ at least partly.
The pulse application device 1 may include a reference laser device that emits laser light of a visible light area in addition to the pulse laser device 10 that emits near-infrared laser light. The reference laser device may be configured to emit reference laser light (continuous wave or pulse) in the visible light region to apply the laser light to the same position as the position on the skin S in which the laser light from the pulse laser device 10 is applied. The reference laser light can be checked visually, which make it easy to check the position on the skin S in which the laser light from the pulse laser device 10 is applied.
The sensor 50 may be an infrared thermometer, a thermography, a color sensor, an image sensor, an acoustic sensor, a power meter, or the like. The pulse application device 1 may include a sensor system including the sensor 50 and a measurement device, such as a spectrum analyzer. For example, the control device 40 may be configured to be capable of executing a computer program enabling arithmetic processing using a trained model that is generated by machine learning, or the like, previously. In this case, the control device 40 may perform arithmetic processing on data that is acquired by the sensor 50 using the trained model and determine a thermal denaturation state of collagen fibers contained in the skin S.
As described above, in the present embodiment, the wavelength of laser light (light) is set within a range in which the temperature rise width of collagen fibers in the skin S when the laser light is applied to the skin S (living tissue) is larger than the temperature rise width of water containing fibroblast (cells) that are contained in the skin and that are present around the collagen fibers.
According to the present embodiment, in the pulse application time period Ton, a rise of the temperature of collagen fibers is set larger than a rise of the temperature of water, which makes it possible to heat collagen fibers more efficiently. Thus, according to such a method, for example, it is possible to obtain more efficient treatment effects than by coagulation of collagen fibers.
In the present embodiment, for example, the cells are fibroblast.
The method of the present embodiment is effective in the case where the cells are fibroblast.
In the present embodiment, for example, the pulse application time period Ton in which a pulse of light is applied to the skin S and the pulse non-application time period Toff in which no pulse of light is applied to the skin S are repeated alternately.
Accordingly, in the pulse non-application time period Toff, it is possible to inhibit the temperature of fibroblast contained in water from rising and eventually inhibit fibroblast from being damaged.
In the present embodiment, for example, the pulse non-application time period Toff (non-application time period) is set such that the temperature of water at the end of the pulse non-application time period Toff is equal to or lower than the first temperature (given temperature).
Accordingly, it is possible more assuredly inhibit a temperature rise of fibroblast and eventually a damage of the fibroblast.
In the pulse application method of the present embodiment, for example, the pulse non-application time period Toff is set such that the temperature of water at the end of the pulse non-application time period Toff is approximately equal to the temperature of water at the start of the pulse application time period Ton.
Accordingly, it is possible to more assuredly inhibit a temperature rise of fibroblast and eventually a damage of fibroblast.
In the present embodiment, the pulse non-application time period Toff is set such that the temperature of collagen fibers at the end of the pulse non-application time period Toff is higher than the temperature of collagen fibers at the start of the pulse application time period Ton immediately before the pulse non-application time period Toff.
Accordingly, it is possible to speedily increase the temperature of collagen fibers by repeating application of a pulse.
In the present embodiment, the pulse non-application time period Toff is set based on the thermal relaxation time period from the end of the pulse application time period Ton immediately before the pulse non-application time period Toff until a time when the temperature of collagen fibers decreases to a temperature obtained by adding the temperature rise width obtained by adding the temperature width obtained by dividing the temperature rise of collagen fibers in the pulse application time period Ton by the bottom of a natural logarithm to the temperature at the start of the pulse application time period Ton.
Accordingly, it is possible to set the pulse non-application time period Toff more appropriately according to the thermal relaxation time period of collagen fibers.
In the present embodiment, the pulse non-application time period Toff is set equal to or more than the thermal relaxation time period of collagen fibers.
Accordingly, it is possible to assuredly inhibit a temperature rise of collagen blast cells and eventually a damage of fibroblast.
In the present embodiment, the pulse non-application time period Toff is between 80 [ms] and 210 [ms] inclusive.
As is clear from
In the present embodiment, the pulse application time period Ton is set such that the temperature of water at the end of the pulse application time period Ton is equal to or lower than the second temperature (given temperature).
Accordingly, it is possible to more assuredly inhibit a temperature rise of fibroblast and eventually a damage of fibroblast.
In the present embodiment, the second temperature is a thermal denaturation threshold temperature at which collagen molecules in collagen fibers thermally denature.
Accordingly, it is possible to thermally denature collagen molecules.
In the present embodiment, the second temperature is a reversible thermal denaturation threshold temperature at which the collagen molecules in the collagen fibers reversibly thermally denature.
Accordingly, it is possible to reversibly thermally denature collagen molecules.
In the present embodiment, the wavelength and the pulse application time period Ton are set such that the collagen molecules in collagen fibers thermally denature and fibroblast are not thermally damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while thermally denaturing collagen molecules.
In the present embodiment, the wavelength and the pulse application time period Ton are set such that collagen molecules in collagen fibers thermally denature and fibroblast are reversibly damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while thermally denaturing collagen molecules.
In the present embodiment, the wavelength and the pulse application time period Ton are set such that collagen molecules in collagen fibers irreversibly thermally denature and fibroblast are not thermally damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while irreversibly thermally denaturing collagen molecules.
In the present embodiment, the wavelength and the pulse application time period Ton are set such that the collagen molecules in collagen fibers irreversibly thermally denature and fibroblast reversibly thermally denature.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while irreversibly thermally denaturing collagen molecules.
In the present embodiment, the wavelength and the pulse application time period Ton are set such that thermal transpiration occurs on the surface of the skin S.
Accordingly, it is possible to give coagulation treatment in deep tissue.
In the present embodiment, the wavelength, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that collagen molecules in collagen fibers thermally denature and fibroblast are not thermally damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while thermally denaturing collagen molecules.
In the present embodiment, the wavelength, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that collagen molecules in collagen fibers thermally denature and fibroblast are reversibly thermally damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while thermally denaturing collagen molecules.
In the present embodiment, the wavelength, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that collagen molecules in collagen fibers reversibly thermally denature and fibroblast are not thermally damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while irreversibly thermally denaturing collagen molecules.
In the present embodiment, the wavelength, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that collagen molecules in collagen fibers reversibly thermally denature and fibroblast are reversibly damaged.
Accordingly, it is possible to inhibit a thermal damage of fibroblast while irreversibly thermally denaturing collagen molecules.
In the present embodiment, the wavelength, the pulse application time period Ton, the pulse non-application time period Toff, and the number of times the pulse application time period Ton is repeated are set such that thermal transpiration occurs on the surface of the skin S.
Accordingly, it is possible to remove shallow tissue and thus give coagulation treatment in deep tissue.
In the present embodiment, the ratio of the temperature rise width of the collagen fibers to the temperature rise width of water when light is applied to the skin S is equal to or larger than 1.1.
As is clear from
In the present embodiment, at the time when the given denaturation state of collagen fibers is detected by the sensor 50 (detector), application of a pulse ends.
Accordingly, advantages that it is possible to inhibit excessive application of light and omit unnecessary application of light are obtained.
In the present embodiment, in the pulse application time period Ton, a plurality of pulses of light are applied intermittently.
Accordingly, the same effect as that in the case where laser light is applied successively in the pulse application time period Ton can be obtained.
In the present embodiment, the wavelength of laser light is set at a wavelength at which the absorption coefficient of collagen fibers is larger than the absorption coefficient of water.
Accordingly, it is possible to efficiently increase the temperature of collagen fibers while inhibiting a temperature rise of the fibroblast in the pulse application time period Ton.
In the present embodiment, the wavelength of light is set at a value longer than 1480 [nm].
Accordingly, it is possible to more efficiently increase the temperature of collagen fibers while inhibiting a temperature rise of the fibroblast in the pulse application time period Ton.
In the present embodiment, the wavelength of light is set equal to or less than 1600 [nm].
Accordingly, it is possible to more efficiently increase the temperature of collagen fibers while inhibiting a temperature rise of the fibroblast in the pulse application time period Ton.
The present embodiment of the disclosure and modifications thereof have been exemplified and the present embodiment and the modifications described above are an example and are not intended to limit the disclosure. The above-described embodiment and modifications can be carried out in other various modes and various types of omission, replacement, combination and change can be made without departing from the disclosure. Specification, such as each configuration and the shape (the structure, type, direction, model, size, length, width, thickness, height, number, arrangement, position, and material) can be changed as appropriate and enabled.
For example, the living tissue is not limited to skin, and it may be, for example, living tissue containing collagen fibers, such as the alimentary tract, cartilage, or bone. Furthermore, cells may be cells other than fibroblast.
The pulse application number-of-times may be set according to the temperature of water or collagen fibers.
When the wavelength is set longer than 1600 [nm], because the absorption coefficient is relatively small and accordingly a light invasion length is relatively long, it is possible to obtain the same function and effect on a deeper part of living tissue.
The disclosure is usable in a pulse application method and a pulse application device.
According to the pulse application method and the pulse application device, it is possible to selectively heat collagen fibers in living tissue while inhibiting heating of cells that are present in the living tissue.
Additional advantages and modifications will readily occur to those skilled in the art. Therefore, the disclosure in its broader aspects is not limited to the specific details and representative embodiments shown and described herein. Accordingly, various modifications may be made without departing from the spirit or scope of the general inventive concept as defined by the appended claims and their equivalents.
| Number | Date | Country | Kind |
|---|---|---|---|
| 2019-207610 | Nov 2019 | JP | national |
This application is a continuation of PCT international application Ser. No. PCT/JP2020/043058 filed on Nov. 18, 2020 which designates the United States, incorporated herein by reference, and which claims the benefit of priority from Japanese Patent Application No. 2019-207610, filed on Nov. 18, 2019, incorporated herein by reference.
| Number | Date | Country | |
|---|---|---|---|
| Parent | PCT/JP2020/043058 | Nov 2020 | US |
| Child | 17661078 | US |
