JP4429930B2 - Gel products - Google Patents

Description

  The present invention relates to a gel product in which a container is filled with a gel containing a volatile agent such as a repellent, insect repellent, fragrance, or deodorant.

  An example of a conventional gel product is known in which a notch is formed in a flange of a cap body (see, for example, Patent Document 1).

  As shown in FIG. 8, the gel product 70 described in Patent Document 1 has a cap 73 attached to a container 72 in which a gel-like medicine 71 is accommodated, and an upper end portion of a flange 74 of the cap 73. Notches 75 and 75 are formed to face each other. The cap 73 has a plurality of ribs 77, 78, 79 on the top surface of the cap body 76, and the plurality of ribs 77, 78, 79 and the cap body 76 form a plurality of volatilization openings 80.

  In such a gel product 70, after the air a flowing in the upper part of the cap 73 flows into the container 72 from the volatilization port 80 of the cap body 76 through the opening 81 of the container 72 and contacts the drug 71, A flow path of air a that flows out from the volatilization port 80 to the upper portion of the cap 73 through the opening 81 is formed, and air b that flows on the side surface of the cap 73 from the notches 75 and 75 of the flange 74 to the cap body. The air b flows into the container 72 through the volatilization port 80 and the opening 81 of the container 72 and comes into contact with the medicine 71, and then flows out of the air b flowing out from the volatilization port 80 to the top of the cap 73 through the opening 81. By forming a distribution channel, the medicine 71 is volatilized outside the cap 73.

Japanese Patent Laid-Open No. 2002-166986 (page 2-5, FIG. 4)

  However, in Patent Document 1, air a flowing into the container 72 from the top of the cap 73 and air b flowing into the container 72 from the side surface of the cap 73 pass through the same volatilization port 80. Volatility is not good.

  In general, this type of gel product does not have sufficient shape retention of the gel-like drug contained in the gel product. If the gel product is deformed during transportation or storage, or falls over, There is a possibility that the medicine may leak to the outside, which may impair the commercial value.

  This invention is made | formed in view of the situation mentioned above, The objective is the gel product which can aim at the improvement of the volatility of a volatile chemical | medical agent, the improvement of the sustainability of volatilization, and the maintenance of the shape retention property of a gel. Is to provide.

The above object of the present invention is achieved by the following configurations.
(1) The gel product according to the present invention is a gel product comprising a gel containing a volatile drug, a container filled with the gel, and a cap attached to an upper part of the container,
The gel strength of the gel is 100 gf / cm ² or more,
A volatilization port is provided on the top plate and side plate of the cap ,
The volatilization opening provided in the side plate forms an upper opening up to the top plate and forms a lower opening up to the vicinity of the upper end of the container .

According to the invention described in (1) above, since the gel strength of the gel is 100 gf / cm ² or more, the shape retention of the gel can be improved and the gel leakage can be prevented. Moreover, since a volatilization opening is provided in the top | upper surface board and side plate of a cap, air can be efficiently taken in and distribute | circulated from both volatilization openings. Thereby, since the air taken into the cap can be easily turned around, it is possible to improve the volatility of the volatile chemical and the sustainability of the volatilization. In addition, the upper opening of the volatilization port provided on the side plate is formed up to the top plate and the lower opening is formed near the upper end of the container, so that air can be efficiently taken in and distributed from the volatilization port provided on the side plate. can do. Thereby, since the air taken into the cap can be easily turned around, it is possible to improve the volatility of the volatile chemical and the sustainability of the volatilization.

(2) The gel product according to the present invention is the gel product according to (1), wherein the size of the volatilization opening provided in the side plate is set to a width of 5 to 20 mm and a side view length of 10 to 30 mm. It is characterized by being.

  According to the gel product of the present invention, the volatility is not good, the problem that the gel is deformed or leaks can be solved, thereby improving volatility, improving volatility of the volatility, and maintaining the shape of the gel. Maintenance of sex.

Hereinafter, embodiments according to the present invention will be described in detail with reference to the drawings.
1 is an external perspective view showing a first embodiment of a gel product according to the present invention, FIG. 2 is a side view of the gel product shown in FIG. 1, FIG. 3 is a longitudinal sectional view of the gel product shown in FIG. FIG. 5 is a longitudinal sectional view showing a modification 2 of the first embodiment, and FIG. 6 is a longitudinal sectional view showing a second embodiment of the gel product according to the present invention. It is.

(First embodiment)
First, with reference to FIG. 1 and FIG. 2, the gel product which is 1st Embodiment of this invention is demonstrated.

  The gel product 10 which is 1st Embodiment of this invention is comprised from the container 11, the cap 12, and the gel 13 containing the volatile chemical | medical agent, The cap 12 is filled in the container 11 with which the gel 13 was filled. Install.

In this embodiment, the gel 13 is a volatile agent (for example, insect repellent, pest repellent, insecticide, fragrance, deodorant, etc.), gelling agent (for example, agar, carrageenan, gellan gum, xanthan gum, etc.), A solvent (for example, water, alcohol, polyhydric alcohol, etc.) and the like are heated and mixed uniformly, filled in the container 11, and then cooled and solidified to produce a gel strength of 100 gf / cm ² or more. If necessary, surfactants (for example, POE hydrogenated castor oil, POE alkyl ether, POE / POP block polymer, SG-3 (manufactured by Matsumoto Yushi)), nonionic systems, aliphatic carboxylates, dialkyl sulfates, etc. Salts, anionics such as alkyl phosphates, cationic surfactants such as alkylamine salts and quaternary ammonium salts, amphoteric surfactants such as alkylbetaines, amine acids, etc.), preservatives (for example, , Parabens, biocides (trade names), etc.), antioxidants (eg, BHT, BHA, polyphenols, vitamins, etc.), colorants (eg, yellow, blue, red, green, purple, orange, etc.), ultraviolet absorbers, You may mix | blend an antifoamer etc.

Volatile chemicals include penny royal oil, lemongrass oil, orange oil, cassia oil, geranium oil, thyme white oil, peppermint oil, hiba oil, pimento oil, fennel oil, peppermint oil, bergamot oil, lavender oil, roux oil It is preferable to use one or more plant essential oils such as eucalyptus oil, and these can impart a blood sucking inhibitory effect in addition to the above uses.
In addition, terpenes such as limonene, pinene, carvone, citronellal, linalool, citral, geraniol, eugenol, and menthol, which are contained as the main components of the plant essential oils, may be used.

The gel 13 is manufactured to have a gel strength of 100 gf / cm ² or more, and this is to improve the shape retention of the gel 13 and prevent the gel 13 from leaking when it falls. However, by increasing the gel strength, there is a possibility that the volatilizing agent contained in the gel 13 is slightly difficult to volatilize. Therefore, by using the container 11 and the cap 12 described below, it is possible to improve volatility and improve volatility of volatilization.

  The container 11 is formed in a thin shape by blow molding of resin, has a flange 14 at the upper end portion, and has an opening 15 on the inner peripheral side of the flange 14. The opening 15 is sealed with, for example, an aluminum seal 16 (see FIG. 3) before shipment and before use, and the seal 16 is removed during use. In addition, since the temperature of the placement surface in summer varies depending on the location and volatility may be affected by the temperature, the container 11 may be provided with legs or stands of at least 1 mm and no more than 10 mm.

  The cap 12 is formed in a thin shape by resin injection molding, and integrally forms a substantially rectangular plate-shaped top plate 17 and a substantially quadrangular prism-shaped side plate 18. A volatilization port 19 is formed, and a slit-shaped volatilization port (hereinafter referred to as a volatilization slit 20) is formed in the side plate 18.

  The volatilization opening 19 is an opening having a shape imitating a petal formed point-symmetrically from the center of the top plate 17 and may be formed with an opening ratio of 30% or more with respect to the area of the top plate 17. However, the aperture ratio is more preferably 30 to 85%.

  Here, when the opening ratio of the volatilization port 19 is 30 to 85%, when the gel product 10 is used, if the volatilization port 19 is present, air can be efficiently taken into the cap 12 and distributed. In order to obtain this effect, the aperture ratio of the volatilization port 19 is preferably 50% or more. On the other hand, if the opening ratio of the volatilization port 19 exceeds 85%, the air flowability and inflow properties become unstable, and the volatility of the volatilization deteriorates.

  A plurality of volatilization slits 20 are formed at a predetermined interval in the width direction of the cap, and the upper opening is formed to the top plate and the lower opening is formed to the vicinity of the upper end of the container. The opening area of the volatile slit 20 is preferably equal to or larger than the opening area of the volatile port 19. Furthermore, the size of the volatilization slit 20 is preferably within a range of 5 to 20 mm in width and 10 to 30 mm in length in side view, but is not limited to this range.

The cap 12 forms a space above the surface of the gel 13 and inside the cap 12 by the top plate 17 and the side plate 18, and the volume of the space only needs to be 120 cm ³ or more. in ^is, but more preferred is more of 120cm ³ ~250cm 3.

  Moreover, since the cap 12 forms the volatilization port 19 imitating a petal on the top plate 17, it is possible to give a design-friendly impression to the user. In addition to the petals, the volatilization port 19 can have an intended design such as animal patterns, graphic characters, characters, and the like.

And as a balance with the volume of the space formed in the gel product 10 comprised in this way and the volatilization port 19 formed in the cap 12, and the volatilization port total area of the volatilization slit 20, in an initial stage of use, space For a volume of 190 to 240 cm ³ , it is preferable to form a volatilization port with a total area of 50 to 70 cm ² .

  As shown in FIG. 3, the cap 12 is attached to the container 11 by fitting a locking projection 21 formed at a substantially central portion in the height direction inside the side plate 18 to the flange 14 of the container 11. . Therefore, the cap 12 and the container 11 are prevented from being easily detached by fitting the cap 12 into the container 11. Further, when removing the cap 12 from the container 11, it is easy to rotate the cap 12 relative to the container 11. Since the side plate 18 is not subjected to great stress, it can be securely attached and detached without damaging the side plate 18.

  The cap 12 is provided on the inner surface of the side plate 18 so as to face the ribs 22, and the rib 22 is connected to the inner side of the outer side edge of the top plate 17 and the inner side of the side plate 18. 18 is formed so as to project inward. Thereby, the combination rigidity of the top plate 17 and the side plate 18 can be increased, and deformation of the cap 12 can be prevented.

  Further, since the cap 12 is provided with the volatilization slit 20 in the side plate 18, the height of the cap 12 is increased, and a large space is formed in the cap 12. Thereby, since the air taken in from the volatilization slit 20 can be made to go around easily, the flowability and inflow property of air, the volatility of the volatilizing agent, and the volatility of volatilization can be improved.

  Moreover, since the cap 12 forms the lower opening of the volatilization slit 20 to the vicinity of the upper surface of the flange 14 that is the upper end of the container 11, the lower opening of the volatilization slit 20 is formed in the gel 13 accommodated in the container 11. Can be approached. Thereby, while making it easy to let external air flow in into the container 11, since much air can be made to contact the gel 13, the circulatory property and inflow property of air, volatility of a volatile chemical | medical agent, and the sustainability of volatilization. Can be improved.

  Further, the cap 12 is formed so that the outer edge portion of the lower end portion of the side plate 18 has a shape substantially equal to the outer edge portion of the maximum width portion of the container 11. As a result, a design that is stable in appearance can be given, and the shielding property of the space can be improved, and by preventing the inflow of air from an unnecessary place by improving the shielding property. Therefore, the air circulation and inflow of the volatilization port 19 and the volatilization slit 20 can be stabilized, and the volatility of volatilization can be further improved.

  Such a gel product 10 is used when the seal 16 attached to the opening 15 of the container 11 is removed and the engaging protrusion 21 of the cap 12 is externally fitted to the flange 14 of the container 11 in use. The Then, outside air flows in from the volatilization slit 20 of the side plate 18 and comes into contact with the gel 13 in the container 11, and the chemical component volatilized from the gel 13 together with the air, the volatilization slit 19 of the top plate 17 or the volatilization slit of the side plate 18. 20 is released to the outside.

Therefore, according to the gel product 10, since the gel strength of the gel 13 is set to 100 gf / cm ² or more, the shape retention of the gel 13 can be improved, and the leakage of the gel 13 at the time of falling or the like can be prevented. In addition, since the volatilization port 19 is provided in the top plate 17 of the cap 12 and the volatilization slit 20 is provided in the side plate 18 of the cap 12, air can be efficiently taken in from the volatilization port 19 and the volatilization slit 20, and the cap 12. A large space can be secured inside. Thereby, since the air taken into the cap 12 can be easily turned around, the air circulation / inflow property, the volatility of the volatile agent, and the volatility of the volatilization can be improved.
In addition, the cap 12 may have an opening degree adjustment function which can change the magnitude | size of a volatilization opening (volatilization slit) according to a use condition. The opening adjustment function includes a method of providing a slide-type member on the cap, a method of attaching an adhesive seal that can be re-adhered to the cap, a method of providing a cap that can be opened and closed by a hinge, and a double-structured cap. And a method of adjusting the opening degree by rotating one of the caps.

  As a first modification of the present embodiment, the cap 12 may be a cap 12a as shown in FIG. The cap 12a includes an inner cap 23 and an outer cap 24, and the inner cap 23 and the outer cap 24 are formed with a plurality of volatilization openings 19 in the top plate 17 and a plurality of volatilization slits 20 in the side plate 18, respectively. The The inner cap 23 and the outer cap 24 are rotatably connected by a pin 25 provided at the center of the top plate, and the volatilization opening 19 and the volatilization slit 20 are opened by rotating the outer cap 24 with respect to the inner cap 23. The degree can be adjusted. In this case, the inner cap 23 and the outer cap 24 are formed in a cylindrical shape.

  Further, as a second modification of the present embodiment, as shown in FIG. 5, the gel product 10 includes a container 11 b so that the gel 13 is fitted into a container 11 b having a height lower than that of the gel 13 and the container 11 b is entirely covered. Alternatively, the cap 12b may be fitted into the cap. The cap 12 b is formed with a plurality of volatilization openings 19 in the top plate 17 and a plurality of volatilization slits 20 in the side plate 18. In this case, since the gel 13 cannot be formed by filling the container 11b, the gel 13 previously formed in a predetermined shape is fitted into the container. Moreover, it is good to make the gel 13 the state wrapped in the packaging material, and to remove a packaging material at the time of use.

(Second Embodiment)
Next, with reference to FIG. 6, the gel product which is 2nd Embodiment of this invention is demonstrated. In addition, about the part which overlaps with 1st Embodiment, the same code | symbol is attached | subjected to a figure, and the description is abbreviate | omitted or simplified.
As shown in FIG. 6, the gel product 30 of the present embodiment includes a cap 12c in which a plurality of volatilization ports 19 are formed in the top plate 17, a container 11c in which a plurality of volatilization slits 20 are formed in the side plate 26, And a gel 13 accommodated in the container 12c, and a cap 12c is fitted and placed in the upper end opening of the container 11c filled with the gel 13.
Since other configurations and operational effects are the same as those of the first embodiment, description thereof will be omitted.

In addition, this invention is not limited to embodiment mentioned above, A deformation | transformation, improvement, etc. are possible suitably.
For example, as the gel, a gel containing plant essential oils is used in the embodiment of the present invention, but the present invention is not limited to this, and any gel containing a volatile chemical can be applied. Good.
In the embodiment of the present invention, the gel is put in the container in advance. However, the present invention is not limited to this, and the gel product can be volatilized by opening the gel wrapped in the packaging material and putting it in the container. It may be in any state.
Furthermore, in the embodiment of the present invention, resin is used for the material of the cap and the container, but considering the influence of heat such as direct sunlight, a heat insulating resin is used for the material or a heat insulating sheet (for example, for the container) An aluminum foil or the like may be attached.

  In addition, the materials, shapes, dimensions, forms, numbers, placement locations, etc. of the container, cap, seal, volatilization port, volatilization slit, etc. exemplified in the above-described embodiment are arbitrary as long as the present invention can be achieved. , Not limited.

  Below, the test done in order to confirm the effect of the gel product 10 (this invention product) of this invention is demonstrated.

  As shown in FIG. 1, the product of the present invention used for each test is composed of a container 11, a cap 12 and a gel 13, and the gel 13 filled in the container 11 has a volatile drug. Use plant essential oils.

Gel 13 contains 8% by weight of plant essential oils (here, mixed with several kinds of blood sucking inhibitory and repellent effects), 1.5% by weight of gelling agent, 15% by weight of surfactant, In addition, the whole was made 100% by weight, and these were heated and mixed uniformly, filled into the container 11, and then cooled and solidified to prepare a gel strength of 250 gf / cm ² . This gel 13 further contains preservatives, deodorants, antibacterial agents, antioxidants, and coloring agents in appropriate amounts.
The various components described above may be selected from those described in this specification.

The cap 12 is provided with a volatilization port 19 simulating a petal on the top plate 17 and a plurality of volatilization slits 20 from the top plate 17 to the side plate 18. The cap 12 has an upper end width of 74.4 mm, a lower end width of 81 mm, and a height of 49.5 mm. In use, the volume of the space formed in the cap 12 is 120 cm ³ .

Volatilization port 19, to the area of about 37.2cm ² of the top face plate 17, formed by 60% in the aperture ratio, i.e., to form an opening of 22.3cm ^2.

  There are three volatilization slits 20 having a width of 7 mm, a side view length of 21.5 mm, 22.70 mm, and 26.0 mm, and 16 are formed on the side surface of the cap 12 with appropriate intervals. In the case of the volatilization slit 20 having a viewing length of 26 mm, the lower opening is formed at a position 2 mm higher than the upper end surface of the flange 14 of the container 11.

[Volatilization test]
In this test, the product of the present invention and two comparative examples are prepared, and the volatilization amount for each 8 days is measured. Further, the comparative example uses a gel product in which the top plate is close to and opposed to the upper end of the container, has a cap without an air inlet on the side surface, and the remaining specifications are the same as those of the product of the present invention. The test volatilization conditions are 27 ° C. and 60% RH no wind. The results are shown in Table 1.

  As a result of the volatilization test, the average volatilization amount of the product of the present invention is 28.99 g, whereas the average volatilization amount of the comparative example is 18.35 g. Therefore, the product of the present invention is 58.0% from the comparative example. It was found that the volatilization amount was improved. Moreover, when the volatilization amount of this-invention goods was continuously measured after this test, it turned out that the volatilization of a volatile chemical | medical agent lasts effectively for 40 days or more.

[Blood absorption inhibition test]
In this test, two cages that were volatilized using the product of the present invention and two cages (comparative examples) where the product of the present invention was not installed were prepared, and the blood absorption rate of the test insects in each cage was calculated. Thus, the blood sucking inhibitory effect of the product of the present invention on the test insect is evaluated. The results are shown in Table 2.

(Test method)
(1) A mouse fixed with a wire mesh bag so as not to move around in a 25 cm cubic metal cage (20 mesh) is hung on the ceiling surface as a blood sucking source, and the cage is covered with a wrap to form a sealed space.
(2) Install the product of the present invention in the center of the cage and start volatilization.
(3) Two hours after the start of volatilization, about 25 test insects (Human striped mosquitoes, female adults) are placed.
(4) Count the number of blood-sucking solids after 1 hour exposure.
(5) During the test, keep the temperature condition at 27 ± 1 ° C. and the humidity condition at 60 ± 10%.
(6) The room where the test gauge is installed shall be under natural ventilation.

  As a result of the blood-sucking inhibitory effect test, the average blood absorption rate of the product of the present invention is 33.0%, whereas the average blood absorption rate of the comparative example is 93.7%. It was found that the plant essential oils having the blood sucking inhibitory effect were effectively volatilized.

[Repellent efficacy test]
In this test, as shown in FIG. 7, two cylindrical members 101 and 102 having a length of 40 cm (φ20 cm) and a single cylinder (B zone) having a length of 22 cm (φ20 cm). Using the test apparatus 105 in which the partition plate 104 is inserted between the member 103 and the cylindrical members 101 and 103, and the test insect staying in the cylinder where the product of the present invention has been volatilized, Repellent efficacy was evaluated. The results are shown in Table 3.

(Test method)
(1) The partition plate 104 is put between the A ward and the B ward, the A ward is sealed, and the product of the present invention is volatilized in the A ward.
(2) In A and C wards, a mouse is fixed with a wire mesh as an attracting source.
(3) Ten minutes after the start of volatilization, the partition plate 104 between the A ward and the B ward is pulled out, and about 50 females of Aedes albopictus are quickly introduced from the inlet of the B ward.
(4) The repelling rate is calculated by counting the number of test insects in the respective cylinders of the A and C sections after 5 minutes.

  As is apparent from Table 3, as a result of the repellent efficacy test, the repellent rate was 87.9% in the first test, and the repellent rate was 67.6% in the second test. Therefore, it was found that the product of the present invention has a repelling rate of 77.8%, and a sufficient repelling effect can be obtained as well as a blood sucking inhibiting effect.

  Moreover, as a result of performing a deodorization test on a malodorous sample (isovaleric acid, ammonia) using the product of the present invention, it was found that a sufficient deodorizing effect was obtained in the same manner as the blood absorption inhibiting effect and the repelling effect.

  Furthermore, as a result of performing antibacterial / antifungal tests against the test bacteria (S. aureus, black mold) using the product of the present invention, sufficient antibacterial / antifungal effects as well as the above blood-sucking inhibitory effect, repellent effect, and deodorant effect Was found to be obtained.

1 is an external perspective view showing a first embodiment of a gel product according to the present invention. It is a side view of the gel product shown in FIG. It is a longitudinal cross-sectional view of the gel product shown in FIG. It is a longitudinal cross-sectional view which shows the modification 1 of 1st Embodiment. It is a longitudinal cross-sectional view which shows the modification 2 of 1st Embodiment. It is a longitudinal cross-sectional view which shows 2nd Embodiment of the gel product which concerns on this invention. It is an external appearance perspective view of the test apparatus used for the repellent efficacy test. It is sectional drawing of the conventional gel product.

Explanation of symbols

DESCRIPTION OF SYMBOLS 10 Gel product 11 Container 12 Cap 13 Gel 14 Flange 15 Opening 16 Seal 17 Top plate 18 Side plate 19 Volatilization port 20 Volatilization slit 21 Locking protrusion 22 Rib

Claims (2)

A gel product comprising a gel containing a volatile drug, a container filled with the gel, and a cap attached to an upper part of the container,
The gel strength of the gel is 100 gf / cm ² or more,
A volatilization port is provided on the top plate and side plate of the cap ,
The volatilization opening provided in the side plate forms a top opening up to the top plate and forms a bottom opening near the upper end of the container . The gel product according to claim 1, wherein a size of the volatilization opening provided in the side plate is set to a width of 5 to 20 mm and a side view length of 10 to 30 mm.

Images