WO1999012581A2

WO1999012581A2 - Wound dressing

Info

Publication number: WO1999012581A2
Application number: PCT/GB1998/002623
Authority: WO
Inventors: Thomas George Eakin
Original assignee: TG Eakin Ltd
Current assignee: TG Eakin Ltd
Priority date: 1997-09-05
Filing date: 1998-09-01
Publication date: 1999-03-18
Anticipated expiration: 2000-03-05
Also published as: EP1011741B1; JP2001515762A; IL134833A0; NZ503091A; AU749131B2; US20020091347A1; AU8877298A; DE69827646T2; GB9718923D0; CA2302420A1; WO1999012581A3; US6559351B1; DE69827646D1; US6649804B2; JP4383652B2; IL134833A; CA2302420C; EP1011741A2; ATE282437T1

Abstract

A wound dressing is formed from a covering release layer, a dressing layer, an indicator layer, a transparent or translucent indicator bonding layer and a transparent or translucent outer covering. The indicator layer contains a dye which changes colour on contact with water. When the dressing layer becomes saturated, water permeates the indicator layer and triggers a colour change. The colour change is visible through the indicator bonding layer and outer covering and shows a carer that the dressing needs to be replaced.

Description

WOUND DRESSING

The present invention relates to wound dressings and, in particular, to occlusion dressings. The wound dressing of the invention has a visible indicator so that a user can see when the dressing and determine whether it should be changed. The saturation colour change, depending on the amount of exudate, may in most cases indicate that a change of dressing is necessary.

Wound dressings are widely used for many types of epithelial wounds and, in general, need to be changed at regular intervals to ensure that the wound and surrounding area remains as clean as possible. Occlusion dressings function by sealing the wound, thus preventing external contamination and keeping the tissue moist, which promotes healing. It is undesirable to change the dressing frequently since this negates the effect of the occlusion principle. However, when the dressing is saturated, it can no longer perform its function effectively. It would therefore be useful if the patient and carers responsible for changing wound dressings could be alerted when a change of dressing is required.

Dressings which indicate when they are saturated are known and one example is the dressing sold by Convetec under the trade mark SignaDRESS. In the SignaDRESS™ dressing, fluid leaks from the wound into an area behind an impermeable outer covering of the dressing causing a blister to become visible. Once the edge of the blister reaches an indicator line marked on the outer surface of the dressing, changing is required. The SignaDRESS™ dressing does, however, have certain disadvantages, the main one being that it is covered by a polymer film which restricts the flexibility of the dressing and prevents it from conforming to the contours of the wound site. In addition, the indicator is merely a blister on the surface of the dressing and may, in some cases, be difficult to read and, if allowed to enlarge, may become a pouch of fluid excessive to the requirements of a healing environment.

The present invention also provides a dressing which indicates when it needs to be changed. However, it functions in a completely different way from the SignaDRESS™ dressing.

In the present invention, therefore, there is provided a wound dressing comprising:

a. a covering release layer; b. a dressing layer; c. an indicator layer; d. a transparent or translucent covering;

characterised in that the indicator layer comprises a non toxic indicator substance, which changes colour on contact with water, mixed with a diluting agent and the bonding layer comprises a water-impermeable mobile sticky polymer capable of bonding the indicator layer to the dressing layer and to the outer covering.

The advantage of die dressing of the invention is that when it becomes saturated and needs to be changed, liquid penetrates into the indicator layer, causing the indicator substance to change colour. The colour change is visible through the indicator bonding layer and the outer covering and so it is obvious to the person responsible that the dressing needs to be changed. In addition, unlike the SignaDRESS™ dressing, the indicator in the dressing of the present invention covers the entire area of saturation of the dressing. This makes it easy to tell if the dressing needs to be changed. Covering release layers for dressings are known and are designed to be loosely attached to the dressing layer and impermeable to microorganisms. Examples of known types of covering release layers include paper with a siliconised surface or paper coated with a polymer. For this invention, polymer coated papers are preferred as they do not tend to leave residues on the dressing, which can be a problem with siliconised covering release layers. Paper coated witii polyethylene has been found to be a particularly suitable covering release layer for use in this invention.

The dressing of the invention may be of any known type, for example an antiseptic- impregnated gel or other type of fibrous medium such as gauze. However, it is very much preferred that the dressing is of the hydrocoUoid type. HydrocoUoid dressings are well known in the art and consist of a fine paniculate powder which gels in the presence of body fluids and/or water. The hydrocoUoid dressing may consist of a powdered gelling substance suspended in a colloidal suspending agent.

Gelling substances which have been used in hydrocoUoid dressings include starch and, more recently, sodium carboxymethylcellulose, pectin and other moisture- absorbing particulate substances. Mixtures of any of these gelling agents may also be used.

The suspending agent should be water impermeable and mobile and it should be chosen such that it does not create an adverse reaction when placed in contact with a wound. Examples of suitable suspending agents include polyisobutylene, which may be mixed with one or more other polymers, such as polyethylene, and some carbohydrates. In some types of hydrocoUoid dressings, the gelling substance and suspending agent have been replaced by a hydrogel. A particularly suitable hydrocoUoid dressing for the present invention is formed from sodium carboxymethylcellulose, alone or with starch or other moisture absorbing particles suspended in polyisobutylene, which may be mixed with polyethylene or other polymers. The exact composition of the hydrocoUoid wUl be chosen to provide the desired degree of moisture retention. One skilled in the art of hydrocoUoid dressings would be aware of how this could be achieved.

The hydrocoUoid dressing slowly absorbs moisture, which is retained in the area of the wound. There is, in many cases, a relationship of proportionality between the thickness of the dressing and d e time taken for it to become saturated. In addition, the permeability of the dressing may be affected if die dressing is sterilised by irradiation.

One of die features of hydrocoUoid dressings, which makes them particularly suitable for use in the present invention, is that the proportions of gelling substance and suspending agent can be chosen so that the dressing is impermeable to moisture untU it become saturated. This means that no moisture reaches the indicator substance until the dressing is saturated and needs to be changed.

In dressings consisting of hydroxymethylcellulose (and optionally starch) suspended in polyisobutylene or a mixture of polyisobutylene and polyethylene, a suitable ratio of gelling substance to suspending agent is about 1:1.

The indicator substance may be placed in small dots on the outer surface of the dressing layer. Alternatively, the indicator layer may comprise a thin layer of a powdered indicator substance, which may be mixed wim a diluent. The diluent is used in order to emphasise me colour change of the indicator substance. Thus, suitable diluents are of a light colour, often white, which wtfl partially conceal d e original colour of die dry indicator substance and make the colour change more noticable when the indicator substance is wet. Diluents which may be used in me dressing of the invention include sodium carboxyme yl cellulose and magnesium carbonate.

Suitable indicator substances include soluble dyes such as 0.25% crystal green, Mercurochrome™, cobalt salt moisture indicator and gentian violet or, alternatively, it would be possible to use any indicator wiώ a colour change activated by enzymic catalytic action, provided diat the appropriate enzyme is also provided in me indicator layer. An example of a system which uses an enzyme-activated colour change is the system used in analysing urine for die presence of glucose. This system employs glucose oxidase, peroxidase and a colourless hydrogen donor and, on contact with glucose, a coloured compound is produced. If glucose, as well as me enzymes, were mobilised in die indicator layer, contact with moisture would allow me components of the system to mix so that the colour change is produced. There are many other enzyme-activated colour change systems and any of these could be used in a simUar manner to the glucose oxidase/peroxidase system.

The covering layer should be impermeable to moisture in order to prevent exudate from leaking from the wound to me outside of me dressing. It should also be capable of bonding me indicator layer to me remainder of the dressing to prevent leakage of the indicator substance. Preferably, me covering layer wUl be extremely flexible so that the dressing wUl conform to the contours of the patient's skin in the area of the wound.

It is greatly preferred that the covering layer of me present invention should, in fact, be composed of two sub-layers, an indicator bonding layer and an outer covering. The particular advantage of this arrangement is that it provides virtually no trauma to me wound since the layers can be chosen to conform to the contours of the skin surface. In addition, die appearance of a dressing having a two-part covering layer has proved to be more acceptable. Bom of the sub-layers should, of course, be transparent or translucent so mat the colour change in the indicator layer is visible.

The function of the indicator bonding layer is, as its name suggests, to bond the indicator layer to me dressing layer and to me outer covering. It may be formed from a mobUe sticky polymer and suitable polymers include those used as suspending agents in a hydrocoUoid dressing. Thus, polyisobutylene has proved to be particularly suitable for use in the indicator bonding layer of the dressing. The indicator bonding layer may be applied as a coating on top of the indicator layer and this wiU usually be the case when polymers such as polyisobutylene are used. Alternatively, however, the indicator bonding layer may be applied as an evaporating solution of a polymer, which acts as a carrier for the indicator. In iis case, care should be taken that the polymer is water permeable so that it does not seal in the indicator and prevent it from being contacted by moisture seeping through the dressing.

The thickness of the indicator bonding layer wUl largely depend on die material of which it consists. Typically, however, the indicator bonding layer wUl be very dim, preferably from about 0.1 mm to 1.0 mm in thickness. Usually the thickness of the indicator bonding layer wUl be from about 0.4 mm to 0.6 mm and most preferably about 0.5 mm.

The covering layer, or when used, the outer covering sub-layer, may have a larger area than me other layers of the dressing and, in the area surrounding these layers, it may be backed with an adhesive which will adhere to the skin surrounding a wound. In diis case, the covering release paper will be of me same area of the outer covering so that it protects the adhesive.

Suitable outer coverings for occlusion dressings are known and, in general consist of thin films of a polymeric material or thin foam films.

However, although any known type of outer covering can be used, a particularly suitable material is a thin, porous, breathable film of low density polyethylene witii smaU perforations spaced at intervals of, for example 0.25 mm. The film wUl typically be of from 1 to 20 μm in thickness. A suitable film is manufactured by Tredgar Films under the trade mark FLEXIFILM and die use of a dressing with this type of film as an outer covering forms a further aspect of the present invention.

In a second aspect of the invention, there is provided a dressing comprising: a. a covering release layer; b. a dressing layer; c. an outer covering;

characterised in tiiat the outer covering is formed from a porous breathable film of low density polyethylene having a thickness of from 1 to 20 μm and perforations spaced at intervals of from 0.1 to 0.5 mm.

The advantage of using this type of film as the outer covering for the dressing of die present invention is that it has little elasticity but the perforations aUow it to conform to any shape without folding or creasing. This means that the dressing can be placed on any part of the body wi out folding it and without putting causing traumatic stress, which frequently causes irritation in the area surrounding die wound and consequent discomfort to the patient. The flexibility of this outer covering also allows die patient some movement. The conformity and lack of stress provided by a dressing wi this type of outer covering is in contrast to die problems which accompany the use of conventional outer coverings. Thin polymer films may be stretchable but, in most cases, their elasticity creates trauma in the wound and surrounding area. Thin foam films are an improvement but still eitiier limit the conformity of the dressing, create trauma or botii.

Suitably the perforations in the film are spaced at intervals of 0.2 mm to 0.3 mm and typically 0.25 mm.

Preferred covering release layers and dressing layers are equivalent to diose of the first aspect of the invention and it is preferred tiiat e dressing also contains the indicator bonding layer of the first aspect of the invention.

The invention wiU now be further described by way of example only with reference to the following drawing in which:

FIGURE 1 is a cross section through a wound dressing of the present invention.

The dressing consists of a covering release layer (10), a dressing layer (12), an indicator layer (14), an indicator bonding layer (16) and an outer covering (18). The covering release layer (10) is formed from paper with polyethylene coat (20) on the surface adjacent the dressing layer (12). The polyethylene coat (12) ensures that the paper is easily detached from the dressing and is impermeable to microorganisms so that the dressing remains sterile.

The dressing layer (12) is a hydrocoUoid dressing of known type. It consists of absorbent particles (22) of sodium carboxymethylcellulose alone or widi starch or other moisture absorbing particles, suspended in a layer (24) of polyisobutylene, which may be mixed wim one or more other polymers, for example polyethylene. The degree of moisture retention of the dressing layer can be manipulated by changing the proportions of sodium carboxymetiiylcellulose, starch and any other moisture absorbing particles present. Polyisobutylene is a mobile polymer, which retains moisture so that the wound does not dry out, and which does not cause an adverse reaction to a patient. The permeabUity of the dressing is proportional to its thickness and may also be affected if me dressing is sterilised by irradiation. Because polyisobutylene is impermeable to moisture, the dressing layer is impermeable until it becomes saturated. However, the weight ratio of carboxymetiiylcellulose to polyisobutylene is chosen such tiiat, when the dressing is saturated, it is possible for moisture to pass through the dressing layer and reach d e indicator layer (14). A suitable ratio would be 1:1.

The indicator layer (14) is powdered gentian violet spread on die outer surface of me dressing layer (12). The gentian violet powder is held in place by the indicator bonding layer (16), which is formed from polyisobutylene or anotiier mobile sticky polymer. Polyisobutylene is water impermeable and so die bonding layer prevents moisture from reaching the outside of the dressing. The bonding layer (16) has a diickness of about 0.5 mm so that it is transparent or translucent.

The outer covering (18) is formed from a flexible thin polyethylene film with holes about every 0.25 mm. A suitable film is marketed by Tredgar Films under die trade mark FLEXIFILM. The polyethylene film has negligible elasticity but me perforations in the film allow it to conform to any shape without folding or creasing.

In operation, the release paper (10) is removed from me dressing and d e dressing is placed over a wound. The dressing is suitable for any wound of the type for which an occlusion dressing is generaUy used. The mobile polymer used in the hydrocoUoid dressing layer (12) and in the indicator bonding layer (16) and, in particular the flexible polyethylene outer covering (18) ensure that the dressing will conform to the shape of the patient's body in die area of die wound. This is particularly useful as it avoids traumatic stress, which frequently causes irritation in e area surrounding the wound and may retard die healing process. In addition, die flexibUity of the dressing means that the patient retains some mobility in the area of the wound. Thus, the dressing can be used even on an area such as a knee or elbow wid out the usual problems of creasing of the dressing, pressure on d e wound and discomfort to the patient.

The hydrocoUoid dressing layer (12) is water impermeable until e dressing becomes saturated and this ensures that d e wound remains moist so that die healing process can progress. When e dressing becomes saturated, however, and requires changing, the hydrocoUoid dressing layer (12) becomes permeable to water. Water passes through the dressing layer (12) and reaches die indicator layer (14) turning the gentian violet dye to a purple colour. This purple colour is visible through the transparent or translucent indicator bonding layer (16) and outer covering (18) and advises the person responsible for attending to e wound tiiat the dressing is saturated and requires changing.

The moisture from the wound does not reach die outer surface of the dressing because die indicator bonding layer (16) is not permeable to water. This means that the patient's clotiies or bedclotiies do not become soiled. In addition, d e water impermeable indicator bonding layer (16) means that any dirt on the outer surface of the dressing will not reach die wound and, further, that the dressing is easy to clean if me outer surface does become soϋed. Thus, die dressing of die present invention has die advantages of being easy to apply to a wound wim little discomfort to a patient and of indicating to a carer when it needs to be changed.

Claims

1. A wound dressing comprising:

characterised in mat the indicator layer comprises a non toxic indicator substance, which changes colour on contact with water, mixed witii a diluting agent and die bonding layer comprises a water-impermeable mobde sticky polymer capable of bonding d e indicator layer to the dressing layer and to die outer covering.

2. A wound dressing as claimed in claim 1, wherein the covering release layer comprises paper with a sϋiconised or polymer coated surface.

3. A wound dressing as claimed in claim 2, wherein the covering release layer comprises paper coated witii polyethylene.

4. A wound dressing as claimed in any one of claims 1 to 3, wherein the dressing is of the hydrocoUoid type.

5. A wound dressing as claimed in claim 4, wherein the dressing layer comprises a gelling substance comprising sodium carboxymethylcellulose, alone or with starch or other moisture absorbing particles in a suspending agent comprising polyisobutylene, optionally mixed witii polyethylene or otiier polymers.

6. A wound dressing as claimed in claim 5, wherein the ratio of gelling substance to suspending agent is about 1:1.

7. A wound dressing as claimed in any one of claims 1 to 6, wherein the indicator substance is placed in small dots on die outer surface of the dressing layer.

8. A wound dressing as claimed in any one of claims 1 to 6, wherein the indicator layer comprises a thin layer of a powdered indicator substance

9. A wound dressing as claimed in claim 7, wherein the powdered indicator substance is mixed witii a dUuent such as sodium carboxymethyl cellulose or magnesium carbonate.

10. A wound dressing as claimed in any one of claims 1 to 9, wherein me indicator substance is a soluble dye or an indicator with a colour change activated by enzymic catalytic action.

11. A wound dressing as claimed in claim 10, wherein the indicator substance is 0.25 % crystal green, Mercurochrome™, cobalt salt moisture indicator or gentian violet.

12. A wound dressing as claimed in any one of claims 1 to 11 , wherein the covering layer is composed of two sub-layers, an indicator bonding layer and an outer covering.

13. A wound dressing as claimed in claim 12, wherein me indicator bonding layer is formed from a mobile sticky polymer such as polyisobutylene.

14. A wound dressing as claimed in claim 13, wherein the indicator bonding layer is applied as a coating on top of the indicator layer.

15. A wound dressing as claimed in claim 12, wherein die indicator bonding layer is applied as an evaporating solution of a polymer, which acts as a carrier for the indicator, wherein the polymer is water permeable.

16. A wound dressing as claimed in any one of claims 12 to 16, wherein the indicator bonding layer is from about 0.1 mm to 1.0 mm in thickness.

17. A wound dressing as claimed in any one of me preceding claims wherein the covering, or outer covering sub-layer, if present, has a larger area than the dressing, indicator and indicator bonding layers of the dressing and, in the area surrounding these layers, is backed witii an adhesive which wiU adhere to die skin surrounding a wound.

18. A wound dressing as claimed in any one of claims 12 to 17, wherein die outer covering is formed from a porous breathable film of low density polyed ylene having a thickness of from 1 to 20 μm and perforations spaced at intervals of from 0.1 to 0.5 mm.

19. A wound dressing comprising: a. a covering release layer; b. a dressing layer; c. an outer covering;

characterised in mat the outer covering is formed from a porous breathable film of low density polyethylene having a thickness of from 1 to 20 μm and perforations spaced at intervals of from 0.1 to 0.5 mm.

20. A wound dressing as claimed in claim 19, wherein the covering release layer and me dressing layer are as defined in any of claims 2 to 6.