Patent Grant
10835140
The present invention relates to a biological electrode tool for acquiring biological signals, such as a vital sensor for obtaining an electrocardiogram and the like.
Bioelectricity generated by a living body, such as a human body, is induced by the activity of the heart, the brain, muscles and the like. A weak voltage produced by the induced bioelectricity can be acquired using a biological electrode tool closely attached to the skin of the living body. The acquisition may be temporary in the case of an electrocardiogram for health checkup, or may continue for a long time in the case of a surgery or health management for healthcare, for example. Accordingly, the state of the heart and the like is diagnosed in accordance with the data to be acquired.
The biological electrode tool typically includes an electrode portion which is attached to the living body to acquire the biological signal, and a lead portion for externally leading the biological signal from the electrode portion (see Patent Documents 1 and 2).
It is desirable that the biological electrode tool is able to fit the skin so as to feel natural and comfortable. Accordingly, it has been proposed to cover the entire areas of the upper and lower surfaces of the electrode portion, except for the portion that contacts the living body, with nonwoven fabric, and to also cover the entire areas of the upper and lower surfaces of the lead portion, except for an external lead-out end portion thereof, with nonwoven fabric (see Patent Document 2, paragraphs 0021 to 0022, and
Patent Document 1: JP-05-36402 Y
Patent Document 2: JP-A-2014-200559
The biological electrode tool including the electrode portion and the lead portion with the upper and lower surfaces thereof covered with the nonwoven fabric may be manufactured by stamping out a biological electrode portion and a lead portion in a plurality of patterns of the biological electrode portion and the lead portion formed on a film (see Patent Document 2, paragraph 0025, and
In this case, a conductive electrode and a conductive lead wire are exposed on the end faces of the stamped-out electrode portion and lead portion. When the exposed conductive portions contact the skin and the like, the detection signal may become unstable and an error may be caused. In addition, the living body (human) may feel uncomfortable.
The lead portion may be as long as 1 m or longer. In this case, the influence of external noise may have to be considered, because the external noise may affect detection accuracy and cause an error.
In light of the above circumstance, a first object of the present invention is to eliminate the exposure of the conductive portion. A second object is to eliminate the influence of external noise.
In order to achieve the first object, according to the present invention, full circumferential peripheries of the nonwoven fabrics on the upper and lower surfaces of the electrode portion and the lead portion are bonded except for the portion that contacts the living body and the external lead-out end portion. According to this configuration, neither the electrode of the electrode portion nor the thin-film lead wire of the lead portion are exposed. Accordingly, the instability in detection signal or an error caused thereby due to the contact of the exposed conductive portion with the skin and the like can be prevented. Further, the living body, such as a human, is prevented from feeling uncomfortable.
In order to achieve the second object, the biological electrode tool according to the present invention is configured to shield external noise by means of a shield layer provided around the lead wire on the entire circumferential surface of the lead portion via an insulating layer. The shield layer may also be provided in the electrode portion. In this case, it goes without saying that the portion that contacts the living body is excluded.
As a configuration of the present invention to achieve the first object, the configuration including: an electrode portion attached to a living body to acquire a biological signal; and a lead portion for externally leading out the biological signal from the electrode portion can be employed. In the configuration, the electrode portion can include an electrode having upper and lower surfaces entire areas of which are covered with a nonwoven fabric having an electrode opening portion on a living body contacting side, and with a nonwoven fabric opposing the nonwoven fabric; the lead portion can also include upper and lower surfaces entire areas of which are covered with the nonwoven fabrics, except for an external lead-out end portion; the nonwoven fabrics on the upper and lower surfaces of the electrode portion and the lead portion can include bonding portions in full circumferential peripheries of the nonwoven fabrics, the bonding portions being bonded via an adhesive layer except for the electrode opening portion and the external lead-out end portion.
In this configuration, the shield layer is provided along the entire length of the lead portion, covering the entire circumference of the lead wire via the insulating layer. The entire area of the shield layer is covered with the nonwoven fabrics. The nonwoven fabrics are bonded in the bonding portion via the adhesive layer. In this way, the shield layer is also prevented from being exposed from the nonwoven fabrics on the upper and lower surfaces. Accordingly, the second object is achieved.
The shield layer makes it possible to send the biological signal obtained by the electrode portion to the measurement equipment while minimizing the entry of external noise. Accordingly, an increase in S/N is achieved, which eliminates the need for a means for increasing S/N. As a result, the cost of the device as a whole can be decreased. In addition, the shield layer is not exposed, either. Accordingly, the living body can be prevented from feeling uncomfortable due to contact.
The nonwoven fabric on the living body contacting side may be coated with adhesive resin, whereby the lead portion can be closed attached to the living body.
The thin-film lead wire may be obtained by forming a metal foil or a vapor-deposited film of Cu (copper), Au (gold), Ag (silver), Al (aluminum), or Ni (nickel), for example, on a sheet (or film) shaped base material. The lead wire may also be manufactured by forming an electrically conductive ink, electrically conductive paste, or electrically conductive adhesive, obtained by dispersing an electrically conductive polymer or electrically conductive filler in a binder, on a sheet-shaped base material. Examples of the electrically conductive polymer that may be used include polyacetylene, polypyrrole, polythiophene, and polyaniline. Examples of the electrically conductive filler include electrically conductive metal powders, such as Cu powder, Ag powder, Au powder, Al powder, and Ni powder. It is also possible to use an electrically conductive filler obtained by plating or coating an electrically conductive material on a core material of the metal powder or resin powder. It is also possible to use a carbon powder or an electrically conductive polymer powder and the like as the electrically conductive filler.
The thickness and width of the thin-film lead wire may be determined arbitrarily as long as its function can be exerted. For example, the thickness may range from 1 to 100 μm, and the width may range from 100 to 5000 μm. It is also possible to apply, for example, a material which includes an electrically conductive material with a diameter of 20 to 100 μm, such as extra-fine copper wire (high-strength wire), carbon nanotube, or metal-plated resin fiber, and which can be molded into a thin shape or a narrow shape, as appropriate. In the present invention, these may also be included in the thin-film lead wire.
Any nonwoven fabric may be used as long as the nonwoven fabric does not have electrically conductivity. For example, polyester resin fiber may be used. The thickness is not particularly limited as long as it does not adversely affect the use of the fabric. For example, the thickness may range from 50 to 3000 μm.
The adhesive material for bonding the upper and lower nonwoven fabrics preferably has high adhesion to the interposed conductive material (electrode, lead wire). More preferably, the adhesive has electric insulation property and/or waterproof property. For example, polyethylene (PE) may be used.
The shield layer may be formed from the same material and by the same method as for the thin-film lead wire. The thickness may also be arbitrarily determined as long as the shield effect can be obtained. The thickness, for example, may range from 0.1 to 1000 μm.
The present invention has the above-described configurations. Accordingly, a biological electrode tool that is comfortable to the skin and that has high detection accuracy can be obtained.
The electrode portion 10 includes an electrode 11 including an Ag paste layer 11a and a silver chloride (AgCl) paste layer 11b which are successively disposed on the nonwoven fabric 30.
The lead portion 20 includes a copper foil electric wire 21 disposed on the nonwoven fabric 30. The copper foil electric wire (lead wire) 21 includes, for example, a copper foil electric wire (see
On opposing surfaces of the upper and lower nonwoven fabrics 30 (hereafter, in
The biological electrode tool A1 having the above configuration may be manufactured as follows. First, as illustrated in
Then, the nonwoven fabric 30b including a hole (a portion that contacts the living body; the electrode opening portion) 13 of a size corresponding to the electrode 11 is thermally fused (thermally adhered) with the lower nonwoven fabric 30a via the adhesive layer 31, with the electrode 11 positioned in the hole 13 (see
In this case, the nonwoven fabric 30 (the nonwoven fabrics 30a, 30b) may be cut into the shape indicated by solid lines in
The biological electrode tool A1 according to the embodiment can be used to obtain an electrocardiogram and the like by, as is conventionally done, attaching the electrode portion 10 to a required position of the human body via electrically conductive gel, and connecting examination equipment (measurement equipment), such as cardiography equipment, to the terminal portion 14.
The biological electrode tool A2 according to the second embodiment can also be used to obtain an electrocardiogram and the like by, as is conventionally done, attaching the electrode portion 10 to a required position of the human body via electrically conductive gel, and connecting the examination equipment, such as cardiography equipment, to the terminal portion 14.
During the formation of the shield layer 40, an electrically conductive layer 41 is provided on the opposing surfaces of the nonwoven fabrics 30a, 30b by coating or attachment of foil, for example. The electrically conductive layer 41, as in the case of the electric wire 21, is provided by a metal foil of Cu, Au, Ag, Al, or Ni; a vapor-deposited film thereof; or an electrically conductive ink, an electrically conductive paste, or an electrically conductive adhesive including an electrically conductive resin or an electrically conductive filler dispersed in a binder. The electrically conductive layers 41 are bonded via an insulating layer 42 including an insulating adhesive 31 of PE, for example. In this case, the insulating layer 42 is at least provided in an area in which the electrically conductive layer 41 may potentially contact the electric wire 21 or the electrode 11 (and not necessarily in the entire areas of the opposing surfaces of the nonwoven fabrics 30a, 30b as illustrated in
The biological electrode tool A3 according to the third embodiment can also be used to obtain an electrocardiogram and the like by, as is conventionally done, attaching the electrode portion 10 to a required position of the living body via electrically conductive gel, and connecting the examination equipment, such as cardiography equipment, to the terminal portion 14. In this case, the shield layer 40 provided around the electrode portion 10 and the entire length of the top and bottom of the electric wire 21 shields external noise, whereby detection accuracy is improved.
The shield layer 40 may be provided only on the lead portion 20 (and may not be provided on the electrode portion 10).
The lead wire (electric wire) 21 and the shield layer 40 may be formed by directly coating the nonwoven fabric 30 with an electrically conductive paste and the like. The biological electrode tools A1 to A3 may be configured to include electrically conductive gel provided on the AgCl layer 11b. In this case, a film provided so as to cover the electrically conductive gel may be removed in use.
The living body side of the nonwoven fabric 30a of the lead portion 20 may be coated with an adhesive resin of urethane resin or acrylic resin and the like, whereby the lead portion 20 can be closely attached to the living body. As a result, the handling of the biological electrode tools A1 to A3 may be improved when attached for a long time, such as for a full day. It goes without saying that the living body includes not only human bodies but also animals such as dogs and cats.
The currently disclosed embodiments are to be considered illustrative in all aspects and are not limiting. It is intended that the scope of the present invention is defined by the appended claims, and that the present invention includes all modifications falling within the scope of the claims and equivalents thereof.
| Number | Date | Country | Kind |
|---|---|---|---|
| 2015-049026 | Mar 2015 | JP | national |
| Filing Document | Filing Date | Country | Kind |
|---|---|---|---|
| PCT/JP2016/056622 | 3/3/2016 | WO | 00 |
| Publishing Document | Publishing Date | Country | Kind |
|---|---|---|---|
| WO2016/143666 | 9/15/2016 | WO | A |
| Number | Name | Date | Kind |
|---|---|---|---|
| 4082086 | Page | Apr 1978 | A |
| 4082087 | Howson | Apr 1978 | A |
| 4353372 | Ayer | Oct 1982 | A |
| 4370984 | Cartmell | Feb 1983 | A |
| 4524775 | Rasmussen | Jun 1985 | A |
| 4539995 | Segawa | Sep 1985 | A |
| 4694835 | Strand | Sep 1987 | A |
| 4763660 | Kroll | Aug 1988 | A |
| 5024227 | Schmid | Jun 1991 | A |
| 5450845 | Axelgaard | Sep 1995 | A |
| 6865409 | Getsla | Mar 2005 | B2 |
| 8750959 | Lindberg | Jun 2014 | B2 |
| 8755859 | Lang | Jun 2014 | B2 |
| 9510762 | Datovech | Dec 2016 | B2 |
| 20030220553 | Axelgaard | Nov 2003 | A1 |
| Number | Date | Country |
|---|---|---|
| 05036402 | Sep 1993 | JP |
| 2013236922 | Nov 2013 | JP |
| 2013248139 | Dec 2013 | JP |
| 2014042707 | Mar 2014 | JP |
| 2014200559 | Oct 2014 | JP |
| Entry |
|---|
| International Search Report dated May 31, 2016 filed in PCT/JP2016/056622. |
| Number | Date | Country | |
|---|---|---|---|
| 20180055399 A1 | Mar 2018 | US |
