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The skin barrier in canine atopic dermatitis

Published 28/06/2024

Written by Yun-Hsia Hsiao

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Progress continues to be made on our understanding of canine atopic dermatitis; this paper looks in particular at the role of the skin barrier and how its dysfunction may contribute to the condition.

Clinical presentation of cAD

Key points

There is some evidence that a defective skin barrier is a key factor in a dog that develops atopic dermatitis (AD).

An individual dog’s skin microbiota is thought to be another major aspect in determining if AD is likely to develop.

Various factors, including secondary bacterial and yeast infections, flea allergy and adverse food reactions, can make AD worse.

A multimodal approach to treatment is often essential to control AD long-term, including a focus on maintaining a healthy skin barrier.

Introduction 

Skin is an amazing structure and the biggest organ of the body. It serves as a vital barrier between the internal organs and the external environment, protecting an individual from foreign substances and contributing to overall health, and the skin epidermis has evolved to become a dynamic structure with homeostatic capabilities that can cope with altering external conditions. This paper will review the role of the skin barrier in relation to canine atopic dermatitis (cAD) and discuss how best to optimize its health.

Epidermal anatomy

The epidermal layer of the skin consists of several tiers of corneocytes, namely (from inside to outside) the stratum basale, stratum spinosum, stratum granulosum, and stratum corneum (SC). The corneocyte is the final product of epidermal keratinization, and in dogs renewal of the epidermis takes about 22 days; new cells originating from the basal layer migrate upwards to replace the outer layer of dead cells. The cells are held together by a lipid matrix, comprising cholesterol, free fatty acids and ceramides which contribute to forming extracellular lipid-enriched lamellar membranes. A commonly used analogy to describe the skin barrier is the “brick wall theory” whereby the SC forms the “bricks”, while the lipid-enriched layers between the cells forms the “mortar” (Figure 1a) 1. The integrity of the SC, particularly the lipid matrix, is important in maintaining the skin barrier function. 

In addition to intercellular lipids, the outermost layer of the SC is coated with a variety of hydrophobic molecules, forming a protective barrier against microbes and allergens. Skin surface function and skin surface lipids have been investigated extensively in atopic dermatitis (AD) of both humans and dogs, and changes in lipid composition (free fatty acids and ceramides) in AD lesional skin and the lamellar conformation are thought to compromise the integrity of the skin barrier (Figure 1b) 2. Although definitive evidence of the relationship between skin barrier dysfunction and the development of cAD is still lacking, a few candidate genes have been associated with defective epidermal barrier integrity in cAD, such as those encoding for the exoskeleton protein plakophilin 2 (PKP2) and filaggrin (FLG) 3. In human medicine, transepidermal water loss (TEWL) and skin hydration (SH) are used to evaluate skin barrier function, treatment efficacy in atopy patients, and assessment of cosmetic products 4. TEWL and SH measurements are often included in clinical trials due to their noninvasive and convenient nature, but these techniques have not yet been standardized for use in dogs. 

“Brick and mortar” stratum corneum model

Figure 1a. The concept of the “brick and mortar” stratum corneum model involves solid building blocks (the cornified layers) held together by a space-filling mortar. Within the skin lipid matrix are peptides known for their antimicrobial properties, keeping the normal flora balanced and suppressing pathogenic bacteria.
© Yun-Hsia Hsiao/redrawn by Sandrine Fontègne

Compromised epidermal barrier may not effectively prevent the penetration of microbes and allergens

Figure 1b. The “bricks and mortar” model lends itself to demonstrating what happens with a compromised epidermal barrier; this leads to reduced ceramide distribution, increased epidermal water loss, and decreased skin hydration. Note that skin lipid barrier defects may not effectively prevent the penetration of microbes and allergens.
© Yun-Hsia Hsiao/redrawn by Sandrine Fontègne

Skin microbiota

Skin is also colonized by a diverse range of microorganisms (bacteria, Malassezia and fungi) known as the microbiota. In recent years, advances in next-generation sequencing have enabled identification of a wide range of cutaneous residents, and the microbiota can vary significantly between different body sites in the same dog. It is notable that it is susceptible to influences from factors such as topical therapy, systemic medications (especially antimicrobials), and even environmental conditions. 

The exposure to a wide-spectrum microbiota during early life contributes to its adaptation to non-harmful microorganisms 5, and reflects the so-called “hygiene hypothesis” of human atopy. This was proposed in 1989 to explain the increasing prevalence of atopic conditions seen in humans; it suggests that a higher incidence of childhood infections might provide protection against the development of atopic diseases in later life. Babies tend to be born with an immune response that is Th (T-helper cell) 2 biased; this can be switched off rapidly postnatally under the influence of microbiological exposure, or can be enhanced by early exposure to allergens. Th2 cells are known to be involved with allergic responses, whereas the Th1 response is essentially mounted against infectious pathogens. Ideally, the two should be in equilibrium; a balanced Th1/Th2 pattern has been observed in infants that are less likely to develop atopic disease in later life. Unfortunately, there is no current research that supports the hygiene hypothesis in AD dogs, but research indicates a lower diversity in the skin microbiome in atopic dogs when compared to healthy dogs, which exhibit a rich diversity in their microbiota 6. Furthermore, when dogs with AD experience acute flares, there is a temporary disruption in the balance of their microbiota (dysbiosis) due to a substantial increase in Staphylococcus spp. However, after antimicrobial therapy and during remission of lesions, TEWL is reduced, and microbial diversity is restored 7

Canine atopic dermatitis 

cAD is a pruritic and predominantly T-cell driven inflammatory skin disease. Its development has a multifactorial pathogenesis, involving a complex interplay between immune dysregulation, skin barrier abnormalities, genetic predisposition, environmental factors and dysbiosis (Figure 2). It is suggested that the environmental factors play a significant role in the development of cAD 3, as a dog’s lifestyle, particularly during puppyhood, has a notable influence on maturation of the immune system. As such, growing up in a rural environment, having a large number of family members, and being in contact with other animals may lower the risk of developing cAD later in life. In addition, there is also an indication that Toxocara canis infection might have a protective effect against Dermatophagoides farina (house dust mite)-induced cAD 3.

Pathogenesis of cAD: interacting factors

Figure 2. There are various interacting factors in the pathogenesis of cAD; despite it being considered a single disease entity, it is imperative to employ diverse therapeutic strategies to manage it effectively.
© Yun-Hsia Hsiao/adapted from (23,24)/redrawn by Sandrine Fontègne

The primary clinical feature of cAD is pruritus, which can present as either a seasonal or non-seasonal pattern. Lesions are commonly found in areas such as the periocular region, around the muzzle, axillae, inguinal region, perianal area, and the extremities (Figure 3). Dogs with cAD may experience recurrent problems such as otitis externa and pododermatitis, which are commonly associated with secondary bacterial infections or an overgrowth of Malassezia. Diagnosing cAD relies on the exclusion of other pruritic skin conditions, especially those that mimic cAD, such as flea infestation/flea bite hypersensitivity, scabies, and adverse food reaction (AFR). Once ectoparasite prevention, diagnostic examinations and food trials have been successfully performed, Favrot’s criteria can be used to establish a clinical diagnosis of cAD (Table 1) 8. For identification of cAD-related allergens, skin testing and IgE serology tests are available, although it should be realized that these tests are only needed if allergen-specific immunotherapy is considered 9.

Table 1. Favrot’s criteria for canine atopic dermatitis. If 5 or more of the criteria are met there is at least an 80% chance that AD is the cause of the pruritus.

  1. Onset of signs under 3 years of age 
  2. Dog living mostly indoors 
  3. Glucocorticoid-responsive pruritus 
  4. Pruritus without lesions (sine materia) at onset
  5. Affected front feet 
  6. Affected ear pinnae 
  7. Non-affected ear margins 
  8. Non-affected dorsolumbar area 
Clinical presentation of cAD: hair loss around the eyes

a

Clinical presentation of cAD: hair loss on the muzzle

b

Clinical presentation of cAD: hair loss on the ventrum

c

Figure 3. The common distribution and clinical presentation of cAD; hair loss around the eyes (a), muzzle (b) and ventrum (c). 
© Yun-Hsia Hsiao

Complicating factors – pyoderma

Staphylococcus pseudintermedius is one of the commensals on the canine skin and an opportunistic pathogen in pyoderma and otitis externa, commonly associated with underlying cAD and/or adverse food reactions 10. Healthy skin has its own defense mechanisms to prevent bacterial overgrowth, such as antimicrobial peptides (AMP), beta-defensins (BDs), and cathelicidins (caths), located in the extracellular spaces of the SC 11. The microbiota and the skin barrier work together to maintain integrity and defend against the external environment. The precise factors contributing to increased susceptibility of dogs with AD to Staphylococcus spp. infections are not fully elucidated. The diagnosis of a bacterial skin infection (superficial folliculitis and pyoderma) is based on the clinical presentation (papules, pustules or epidermal collarettes – Figure 4) and the presence of intracellular cocci on cytology. Effective management of secondary bacterial infections can be accomplished through topical treatments. Maintaining skin and coat hygiene by shampooing can be particularly beneficial for dogs with cAD, as it helps promote a healthy skin barrier. Shampooing diminishes the allergens attached to the skin surface or hair coat, preventing further irritation. Moreover, in-vitro studies suggest that shampoo or mousse preparations that include antiseptic ingredients can have residual effectiveness for up to 14 days 12, so products containing chlorhexidine, benzoyl peroxide, ethyl lactate, povidone iodine or triclosan may be beneficial in treating superficial pyoderma 13. These should be used 2-3 times weekly, and then tapered down to once a week if the lesions resolve 13. In addition, mupirocin and fusidic acid are recommended as topical antimicrobial agents, due to the lower risk of developing multidrug-resistant S. pseudintermedius (MRSP). Systemic antimicrobial therapy should only be considered if topical treatment proves ineffective or if the infection’s depth and location exceed the scope of topical therapy, with antibiotics selected on the basis of bacterial sensitivity tests. In general, the treatment course should be continued for 2 weeks after remission of the lesions. However, due to the global emergence of MRSP, it is highly advisable to prioritize topical treatments over repeated systemic antimicrobial therapy if the patient’s condition allows. 

Common clinical signs of superficial bacterial infection secondary to atopic dermatitis: Papules

a

Common clinical signs of superficial bacterial infection secondary to atopic dermatitis: pustules

b

Common clinical signs of superficial bacterial infection secondary to atopic dermatitis: erythematous collarettes

c

Figure 4. Papules (a), pustules (b) and erythematous collarettes (c) are all common clinical signs of superficial bacterial infection secondary to atopic dermatitis.
© Yun-Hsia Hsiao

Complicating factors – Malassezia 

Malassezia pachydermatis is a lipid-dependent yeast found on the skin surface. Excessive surface lipids, disruptions in the SC barrier function, and an aberrant immune reaction in cAD may contribute to overgrowth of this opportunistic pathogen 14. Colonization in puppies occurs in a similar fashion to that of Staphylococcus spp., with transmission through licking and nursing by the mother at the very early stages of life. When the conditions are favorable, Malassezia can proliferate within the SC, producing numerous antigens and allergens 14. These antigens can penetrate the epidermis and trigger an immune response in cAD dogs, resulting in pruritus and erythema. Malassezia tends to flourish in areas of the skin with high humidity, such as skin folds around the ears, lips, anus, axillae, inguinal region and the claws/interdigital areas. Clinical presentations may manifest as pruritus and erythema, accompanied by malodor or a greasy skin coat. There is no gold standard for diagnosing Malassezia dermatitis, but skin cytology and a compatible clinical presentation are the most effective methods; culture, histopathology and IgE tests lack substantial clinical diagnostic value. 

The primary treatment options consist of antifungal agents such as topical imidazoles, clotrimazole, climbazole, and miconazole. Terbinafine and 2% chlorhexidine/2% miconazole shampoo are alternatives. However, although antiseptic ingredients can substantially diminish a Malassezia overgrowth, emollient bathing products containing cleansing oils, and emollient shampoos with a ceramide-based moisturizer have also demonstrated similar clinical efficacy 15.

Complicating factors – fleas and adverse food reactions 

Flea control and elimination of food allergens are vital strategies in managing cAD, as these help to lower the threshold for pruritus, ultimately improving the patient’s quality of life. Oral adulticides are indicated for efficient year-round control of fleas, as shampooing can flush out topical products and reduce their effectiveness. Isoxazoline products have demonstrated a rapid onset of efficacy, being able to eliminate fleas within 24 hours of administration, which prevents further flea bites. 

Adverse food reactions can coexist with cAD, with estimates ranging from 9-50% among dogs displaying lesions indicative of cAD. To differentiate AFR and atopic dermatitis (which is mainly due to environmental allergens) a strict 8-week food trial based on a novel or hydrolyzed protein diet must be followed. It is also advisable to consider provocative testing after the food trial in order to identify specific food allergens and subsequently remove them from the dog’s daily diet. Although the exact immune mechanism of AFR is not fully understood, a study in affected dogs that had shown significant clinical improvement on an elimination diet trial reported that 90% went on to display clinical signs again (pruritus, feet licking, face rubbing) when tested subsequently, some within a few hours of being fed the provocative diet 16

Yun-Hsia Hsiao

It is suggested that environmental factors play a significant role in the development of cAD. A dog’s lifestyle, particularly during puppyhood, has a notable influence on the maturation of the immune system.

Yun-Hsia Hsiao

Control and management of cAD

cAD is a skin disease which cannot be cured, and it usually requires life-long management customized for the individual patient. Allergen-specific immunotherapy (ASIT) is considered the specific treatment, involving injections of increasing concentrations of environmental allergens identified by skin testing and IgE serology. The clinical effectiveness of ASIT is approximately 60% and may require 9-12 months treatment before noticeable improvement 17. Recently, intralymphatic and sublingual immunotherapy options have been introduced as alternatives to the traditional subcutaneous injection method; these offer a more rapid induction, and the former method is needle-free 18. However, it is essential to manage the pruritus and skin lesions continuously until clinical signs are alleviated through ASIT. Management of cAD depends on the stage of the disease – so for example, rapid intervention with acute flares, control of the chronic disease, or prevention of relapses. As pruritus is the key sign of AD and skin lesions are common secondary to this, treatment should be focused on diminishing the itch. Depending on the intensity of the pruritus, and the distribution and extent of the lesions, topical and/or systemic medication can be chosen. To control acute flares glucocorticoids (topical and systemic) and oclacitinib are considered to be the most effective because of their rapid action, although glucocorticoids are noted for potential adverse effects, which may include polyuria, polydipsia, polyphagia, increased susceptibility to infections, and iatrogenic hyperadrenocorticism. Long-term or high-dose use of glucocorticoids should be carefully monitored, with a switch to other regimes if possible. When the skin lesions have reduced to a mild level, oclacitinib is preferred for its effectiveness in managing residual pruritus and mild flares, as it diminishes the pruritogenic signaling pathway and pro-inflammatory cytokines. However, after the initial two week twice daily initiation phase, patients will often show a rebound phenomenon when tapered to once daily treatment 19. In order to prevent this, topical hydrocortisone aceponate can be added as combination therapy 20

These regimes can be considered as reactive therapy, primarily to be used during ongoing flares or for pruritus management. Once the skin condition is under control, the treatment should be shifted, using narrow-target drugs which are less impactful to the individual, typically cyclosporine and tacrolimus. Cyclosporine is a calcinurin inhibitor which binds to lymphocyte cytoplasm, inhibiting activation of T cells and its down-regulation mediators. Nevertheless, the introduction of cyclosporine takes 2-4 weeks for clinical efficacy, but because of its prolonged half-life, patients have a better chance of tapering down to a lower frequency compared to other medications. It is considered safe for long-term administration, although patients may suffer from initial transient adverse effects such as vomiting and diarrhea; these usually resolve spontaneously without further treatment. Tacrolimus ointment does not cause the adverse reactions (e.g., skin atrophy or comedones) that are observed with topic glucocorticoids, but mild irritation might be noticed in some dogs. In well-managed cases, lokivetmab (a monoclonal antibody that targets interleukin (IL)-31, a common pruritus mediator in patients with cAD) is recommended as proactive therapy 21. The concept is to consistently diminish the residual subclinical inflammation that could potentially trigger sudden flares. 

To prevent recurrence of cAD, direct restoration of the skin barrier function is another important factor, and oral essential fatty acid (EFAs) or fatty acid-enriched diets have been used for many years. EFAs have been demonstrated to reduce the medication score and pruritus in AD dogs over a 9-month duration 22, but antihistamines and probiotics have exhibited insufficient evidence to support their use as treatment options for cAD. 

Conclusion 

Canine atopic dermatitis (cAD) is a chronic relapsing pruritic skin disease that is commonly seen in veterinary practice. The pathogenesis is linked to the disruption of the skin barrier; genes associated with a defective stratum corneum, the microbiota and environmental factors influencing immune balance are all connected to its development. Treatment regimens and strategies have undergone significant progress over the past decade, but a proper diagnosis is the first step in managing the cAD patient. Concurrent bacterial and/or yeast infection may compromise treatment efficacy, and ultimately the choice of therapy depends on the phase and severity of the condition. Although atopic dermatitis is not curable, a multimodal approach can give the dog a good quality of life, and ensuring a healthy skin barrier should help prevent further exacerbations of pruritus and inflammation. 

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Yun-Hsia Hsiao

Yun-Hsia Hsiao

Dr. Hsiao obtained her veterinary degree from Chia-yi University and went on to complete a Master’s program in surgery at Chung-Hsing University in Taiwan Read more