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  2. Skin scarring
  3. Skin scarring
Clinical Review

Skin scarring

BMJ 2003; 326 doi: https://doi.org/10.1136/bmj.326.7380.88 (Published 11 January 2003) Cite this as: BMJ 2003;326:88
  1. A Bayat, specialist registrar in plastic and reconstructive surgerya (ardeshir.bayat{at}man.ac.uk),
  2. D A McGrouther, professor of plastic, reconstructive and hand surgerya,
  3. M W J Ferguson, professorb
  1. a Department of Plastic and Reconstructive Surgery, South Manchester University Hospital Trust, Wythenshawe Hospital, Wythenshawe, Manchester M23 9LT
  2. b Division of Cells, Immunology and Development, School of Biological Sciences, University of Manchester, 3.239 Stopford Building, Manchester M13 9PT
  1. Correspondence to: A Bayat

    Deciding whether to treat a scar or leave it alone depends on accurate diagnosis of scar type and scar site, symptoms, severity, and stigma

    Each year in the developed world 100 million patients acquire scars, some of which cause considerable problems, as a result of 55 million elective operations and 25 million operations after trauma.1 There are an estimated 11 million keloid scars and four million burn scars, 70% of which occur in children.1 Global figures are unknown but doubtless much higher. People with abnormal skin scarring may face physical, aesthetic, psychological, and social consequences that may be associated with substantial emotional and financial costs. This article reviews the spectrum of abnormal scar types, a range of problems associated with scarring, and provides advice on assessment, treatment, and new therapeutic developments.

    Summary points

    Skin scars are the normal and inevitable outcome of mammalian tissue repair

    Skin scarring covers a wide spectrum of clinical phenotypes from normal fine lines to abnormal widespread, atrophic, hypertrophic, and keloid scars and scar contractures.

    Abnormal scars can cause unpleasant symptoms and be aesthetically distressing, disfiguring, and psychosocially and functionally disabling

    Appropriate treatment depends on scar type and aetiology. Options vary from leaving alone to using a combination of corticosteroids, surgical excision, and radiotherapy

    Recent advances in understanding of the biological basis of embryonic skin healing has led to the development of new drugs to prevent scarring

    Method

    This article is based on our scientific and clinical experiences in dermal scarring and on selected articles in recent issues of journals on plastic and reconstructive surgery, dermatology, and wound healing. Key terms included keloid disease, hypertrophic scars, and contractures, plus diagnosis, prevention, and treatment.

    Why do we scar?

    Scars are the end point of the normal continuum of mammalian tissue repair. The ideal end point would be total regeneration, with the new tissue having the same structural, aesthetic, and functional attributes as the original uninjured skin. Scarless skin healing occurs in early mammalian embryos,2 and complete regeneration occurs in lower vertebrates, such as salamanders, and invertebrates.3

    What, if any, are the advantages of scarring, and why do we scar? We hypothesise that wound healing is evolutionarily optimised for speed of healing under dirty conditions, where a multiply redundant, compensating, rapid inflammatory response with overlapping cytokine and inflammatory cascades allows the wound to heal quickly to prevent infection and future wound breakdown. A scar may therefore be the price we pay for evolutionary survival after wounding.

    Skin scarring: the clinical problem

    Scars arise after almost every dermal injury—rare exceptions include tattoos, superficial scratches, and hopefully venepunctures. Scars are often considered trivial, but they can be disfiguring and aesthetically unpleasant and cause severe itching, tenderness, pain, sleep disturbance, anxiety, depression, and disruption of daily activities.4 Other psychosocial sequelae include development of post-traumatic stress reactions,5 loss of self esteem,6 and stigmatisation,7 leading to diminished quality of life. Physical deformity as a result of skin scar contractures can be disabling.8 Many scars take two to three years to pale and mature.

    In spite of media suggestions to the contrary, scars cannot yet be made to disappear. Many patients arrive at plastic surgery clinics with unrealistic expectations. Clinical judgment is required when considering treatment, balancing the potential benefits of the various treatments available against the likelihood of a poor response and possible iatrogenic complications. The evidence base for the use of many current treatments is poor, and some may have only placebo benefit.

    There is considerable quantitative and qualitative variation in scarring potential between individuals and even within the same individual9: scars are normally worst in the deltoid and sternal regions and best in intraoral tissues, reflecting biological and mechanical differences between such sites. Injury in adolescents and young adults normally results in worse scarring than does similar injury in elderly people, reflecting the altered inflammatory and cytokine profile of old wounds, which in many respects resemble those of the early embryo.10 Individuals with pigmented skin are more prone to severe skin scarring than white people.11

    The spectrum of skin scar types

    Skin tissue repair results in a broad spectrum of scar types, ranging from a “normal” fine line (fig 1) to a variety of abnormal scars, including widespread scars, atrophic scars, scar contractures, hypertrophic scars, and keloid scars.

    Fig 1
    Fig 1

    A fine line scar in forearm of a white man after a knife wound

    Widespread (stretched) scars appear when the fine lines of surgical scars gradually become stretched and widened, (fig 2) which usually happens in the three weeks after surgery.9 They are typically flat, pale, soft, symptomless scars often seen after knee or shoulder surgery.12 Stretch marks (abdominal striae) after pregnancy are variants of widespread scars in which there has been injury to the dermis and subcutaneous tissues but the epidermis is unbreached. There is no elevation, thickening, or nodularity in mature widespread scars, which distinguishes them from hypertrophic scars.

    Fig 2
    Fig 2

    Widespread scar (A) in the midline after surgical incision and a hypertrophic scar (B) after transverse surgical incision in an Asian woman

    Atrophic scars are flat and depressed below the surrounding skin. They are generally small and often round with an indented or inverted centre (fig 3), and commonly arise after acne or chickenpox.13

    Fig 3
    Fig 3

    Atrophic scars after acne in upper back and shoulder area of a white man

    Scar contractures— Scars that cross joints or skin creases at right angles are prone to develop shortening or contracture. Scar contractures occur when the scar is not fully matured, often tend to be hypertrophic, and are typically disabling and dysfunctional (fig 4). They are common after burn injury across joints or skin concavities.

    Fig 4
    Fig 4

    Scar contracture of forearm and wrist after a burn injury to a white woman

    Raised skin scars

    Raised skin scars are described as hypertrophic or keloid scars.14

    Hypertrophic scars are raised scars that remain within the boundaries of the original lesion, generally regressing spontaneously after the initial injury (fig 5).15 Hypertrophic scars are often red, inflamed, itchy, and even painful. They typically occur after burn injury on the trunk and extremities.

    Fig 5
    Fig 5

    Presence of multiple scar types in same anatomical site of a white woman after surgery—widespread scar (A), hypertrophic scar (B), and keloid scar (C)

    Keloid scars are raised scars that spread beyond the margins of the original wound and invade the surrounding normal skin in a way that is site specific. Ear lobe keloids often grow as large lobules (fig 6), central sternal keloids commonly develop a butterfly shape, and deltoid keloids tend to extend vertically. A keloid continues to grow over time, does not regress spontaneously, and almost invariably recurs after simple excision. It is difficult to apply the term keloid until a scar has been present for at least a year, although there is no precise time interval. Histologically, keloids have a swirling nodular pattern of collagen fibres.16

    Fig 6
    Fig 6

    Right ear keloid scar after reduction surgery for prominent ears in a white man

    Scars that are difficult to categorise have been termed intermediate scars.17 However, if a raised scar is still emerging after a year, a true keloid is a potential diagnosis, whereas hypertrophic scars should show some evidence of regression within this time. Keloids may be inflamed, itchy, and painful, especially during their growth phase. Common presentations are in the ear lobe after ear piercing, the deltoid after vaccination, and the sternum after acne, chickenpox, trauma, or surgery. Keloids are unique to humans, and there seems to be some genetic predisposition, with dark skinned races being more prone to them, though there are few large epidemiological studies. They develop predominantly in people aged 10–30 years, with an apparent predilection for emergence and deterioration during puberty and pregnancy.11

    Structured scar assessment

    Accurate scar assessment is essential for diagnosis and for starting, monitoring, and evaluating a therapeutic strategy for scar management. The cause and course of scar development are important—is the scar getting better or worse? A decision whether to treat will depend on:

    1. Site (anatomical location of the scar)

    2. Symptoms (pain, itching, etc)

    3. Severity of functional impairment (such as joint mobility)

    4. Stigma (how much is the patient disturbed?)

    The severity of scars is often judged by eye but can be assessed quantitatively with a scar assessment guide such as the Vancouver scar scale18 or the Manchester scar proforma, a validated method for scar assessment and monitoring (see example on bmj.com). The exact anatomical location of scars are recorded, as are their number and size per site and a description of their margins, surface, colour, and texture.19 From these a score is compiled, with the lower the score the better the scar. A standardised colour photograph of the scar lesion at each consultation provides a reference to evaluate effectiveness of treatment since changes occur slowly.

    The presence of a positive family history, previous abnormal scarring in the same or other anatomical sites, poor response to treatment or recurrence of scarring, specific anatomical locations (such as the sternum), large size, prolonged inflammation, and severe symptoms are associated with abnormal scarring.

    Current methods of treating problematic scars

    A simple plan of treatment can be offered with three courses of action—non-invasive treatment, invasive treatment, and leave alone management (fig 7).

    Fig 7
    Fig 7

    Flow chart for managing scars from diagnosis to treatment

    Non-invasive options include use of compression therapy (such as pressure garments with or without gel sheeting); static and dynamic splints; acrylic casts; masks and clips; application of a variety of oils, lotions, and creams; antihistamine drugs; hydrotherapy; and psychosocial counselling and advice. 20 21 Silicon sheeting, with or without adhesive, has become popular.22 Massage therapy is often advocated but lacks evidence of benefit. All the above treatments are empirical.22 Without proper trials, benefits are difficult to quantify objectively, although even a placebo benefit may be appreciated by patients.

    Invasive treatments include surgical excision and resuture. Generally, revision should be considered only if the surgeon thinks that more favourable conditions for wound healing can be provided than on the first occasion (less inflammation, better technique). Intralesional corticosteroid injection20 is widely used but is prone to complications (fat atrophy, dermal thinning, and pigment changes). Other treatments that have been advocated with variable outcomes include injections of fluorouracil,23 interferon gamma,24 and bleomycin,25 radiotherapy,26 laser therapy,27 and cryosurgery.28

    Additional educational resources

    Most scientific and clinical papers on scarring are published in journals of plastic and reconstructive surgery, dermatology, and specific wound healing. Examples include:

    BMJ archive

    Harding KG, Morris HaotL, Patel GK. Science, medicine, and the future: healing chronic wounds. BMJ 2002;324:160-3

    Useful websites
    Recommended reading
      1. Clark RAF
      . Molecular and cellular biology of wounds. 2nd ed. London: Plenum Press, 1996
      1. Morris PJ,
      2. Wood WC
      1. Cherry GW,
      2. Hughes MA,
      3. Leaper DJ,
      4. Ferguson MWJ
      . Wound healing. In: Morris PJ, Wood WC eds. Oxford textbook of surgery. 2nd ed. Oxford: Oxford University Press, 2001:12959
      1. Garg HG,
      2. Longaker MT
      eds. Scarless wound healing. New York: Marcel Dekker, 2000:21326
      1. Champion RH,
      2. Burton JL,
      3. Burns DA,
      4. Breathnach SM
      1. Ferguson MWJ,
      2. Leigh IM
      . Wound healing. In: Champion RH, Burton JL, Burns DA, Breathnach SM eds. Textbook of dermatology. 6th ed. Oxford: Blackwell Science, 1998:33756
      1. Ferguson MWJ,
      2. Whitby DJ,
      3. Shah M,
      4. Armstrong J,
      5. Siebert JW,
      6. Longaker MT
      . Scar formation: the spectral nature of fetal and adult wound repair. Plast Reconstr Surg 1996;97:85460
      OpenUrlCrossRefPubMedWeb of Science

    Leave alone management— Most scars are best left undisturbed by invasive treatment for a year to mature before any judgment is made on their appearance. Monitoring (wait and watch) will allow ongoing assessment of appearance, symptoms, and psychological impact, and reassurance is important. Some scars are best left alone in the long term. Informed, shared decision making with patients may help reduce inappropriate demands for treatment.

    When such management plans are applied to specific scar types, certain patterns emerge:

    • Treatment of widespread scars is mostly by revision surgery to narrow the width of the scar. Revised scars in anatomical sites subject to excessive tissue mobility such as limbs can benefit from splinting29

    • Atrophic scars have been improved with chemical peels, cutaneous laser resurfacing, dermabrasion, punch excisions, and the use of soft tissue biological and alloplastic biological fillers30

    • It is important to distinguish between hypertrophic and keloid scars as inappropriate management can lead to recurrence and larger scars. Simple surgical excision of keloid scars has a 50%-80% risk of recurrence.31 A combination of surgery with either intralesional corticosteroid injection or radiotherapy has been the mainstay of treatment32

    • For scar contractures, surgical release with splinting, acrylic casting, and compression therapy may be required. Full thickness and split or partial thickness skin grafts and, perhaps more effectively, local and free flaps are used for reconstruction of difficult and extensive scars and contractures.33

    Future perspectives

    By subtly altering the regulatory growth factor cascades involved in wound healing—for example, increasing the ratio of cytokines such as transforming growth factor β3 compared with factors β1 and β2—the endogenous embryonic regenerative response can be restored without any adverse consequences on wound strength, healing rates, or incidence of wound infection.3436 Transforming growth factor β3, neutralising antibodies to transforming growth factors β1 and β2, and mannose-6-phosphate are all in early stage human clinical trials for preventing skin scarring. Thus, future drug treatments hold the promise of substantially improving the cosmetic outcome of injury, trauma, or elective surgery, with scarring no longer being an inevitable consequence of skin healing.

    Acknowledgments

    Research summarised in this manuscript has been supported by a variety of grants from the MRC, Wellcome Trust, and the Biotechnology and Biological Sciences Research Council. AB is an MRC fellow.

    Footnotes

    • Competing interests MWJF is the co-founder and chief executive officer of Renovo. DAMcG is a member of the scientific and clinical advisory board of Renovo.

    • Embedded Image

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