Abstract
There are many rheumatic diseases presenting with skin manifestations. This could be the first presenting feature of a systemic rheumatic disease. In addition, some of these skin manifestations could be an indication of an active disease or a sign of a serious medical emergency. In this chapter the skin manifestations of common rheumatic diseases will be described. Particular focus will be placed on rheumatic diseases with polyarthritis. The differential diagnosis of erythema nodosum will be discussed as this condition is observed in several disorders with arthritis. There are many drugs used in rheumatology. Some of them like allopurinol can lead to life-threatening dermatological conditions. A quick review on some of these conditions will be outlined. At the end of this chapter, the reader should be able to recognize different dermatological signs associated with patients with arthritis, discuss the differential diagnosis of erythema nodosum, and recognize life-threatening dermatological conditions.
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1 Introduction
There are many rheumatic diseases presenting with skin manifestations. This could be the first presenting feature of a systemic rheumatic disease. In addition, some of these skin manifestations could be an indication of an active disease or a sign of a serious medical emergency. In this chapter the skin manifestations of common rheumatic diseases will be described. Particular focus will be placed on rheumatic diseases with polyarthritis. The differential diagnosis of erythema nodosum will be discussed as this condition is observed in several disorders with arthritis. There are many drugs used in rheumatology, some of them like allopurinol can lead to life-threatening dermatological conditions. A quick review on some of these conditions will be outlined. At the end of this chapter, the reader should be able to recognize different dermatological signs associated with patients with arthritis, discuss the differential diagnosis of erythema nodosum, and recognize life-threatening dermatological conditions.
2 Objectives
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To identify the dermatological signs in patients presenting with polyarthritis.
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To construct a diagnostic approach to patients presenting with erythema nodosum.
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To recognize life-threatening dermatological conditions.
3 Polyarthritis with Skin: (Diagram 15.1)
3.1 Rheumatoid Arthritis (RA)
RA is a chronic inflammatory disorder that affects the joints and causes symmetrical arthritis. It usually involves extra-articular structures like the skin, eye, lung, heart, kidney, blood vessels, and bone marrow. The skin manifestations of RA will be discussed here.
3.2 Pyoderma Gangrenosum
It presents as an inflammatory and ulcerative disorder of the skin. It’s an uncommon neutrophilic dermatosis. It presents commonly as an inflammatory papule or pustule that progresses to a painful ulcer; it may also present with bullous, vegetative, peristomal, and extracutaneous lesions.
3.3 Rheumatoid Vasculitis
Inflammation of blood vessel is a central feature of RA, and it is considered as one of the primary events in the formation of rheumatoid nodule. Histologically it is characterized by mononuclear cell cuffing of postcapillary venule. It occurs in patients with long-standing joint-destructive RA. It affects vessels from medium vessel to small arterioles; it leads to ischemia and necrosis to blood vessel “occlusion.”
3.4 Rheumatoid Nodule
It is one of the most common cutaneous manifestations in RA. The nodule is seen on pressure area such as olecranon process and many other areas in the body. It is firm, with size varies between 2 mm and 5 cm; non-tender and moveable in subcutaneous tissue; it could be painful, interfere with function, and may cause neuropathy [ 1 ]. Around 75% of patients with Felty’s syndrome have a nodule [1], and a vast majority of patient with nodule have positive RF [2]. Patients with nodule are more likely to have vasculitis [3] (Figs. 15.1 and 15.2).
3.5 Skin Ulceration
It may result from venous stasis, vasculitis, arterial insufficiency, and neutrophilic infiltration [4].
There are many cutaneous changes that occur in patients with RA such as granulomatous dermatitis and medication-induced skin changes, and also there are rare manifestations as linear bands or annular lesions, urticarial eruption, erythema elevatum diutinum, and dermal papule.
3.6 Systemic Lupus Erythematosus (SLE)
The dermatological manifestations are the most common presentation of SLE in general. They involve the skin, mucous membranes, and hair. The new classification criteria of SLE contains acute cutaneous lupus erythematosus (ACLE) lesions, subacute cutaneous lupus erythematosus (SCLE), and chronic cutaneous lupus erythematosus as follows.
3.7 ACLE (Localized)
3.7.1 Malar Rash
Characterized by erythematous butterfly-shaped rash over the cheeks and nasal bridge sparing the nasolabial folds, it can be flat or raised, painful, and lasting for days to weeks [5].
3.7.2 Disseminated (Generalized) ACLE
This lesion is characterized by erythematous to violaceous, scaly maculo-papular widespread exanthum symmetrically involves trunk and extremities. Other nonspecific lesions can be seen, for example; subungual erythema, ulcers, pitting scars stubby hair cheilitis, periorbital edema, and diffuse telogen effluvium [5].
3.7.3 SCLE
The clinical fissures of this type are characterized by circulating anti-Ro and anti-La antibodies and the HLA-B8 and HLA-DR3 haplotype. There are two variants that have been identified: annular variant and papulosquamous variant. The annular variant contains slightly raised erythemas with central clearing, while the papulosquamous variant consists of psoriasis-like or eczematous-like lesions. These two variants usually involve UV-exposed skin, including the lateral aspects of the face, the “V” of the neck, the upper ventral and dorsal part of the trunk, and the dorsolateral aspects of the forearms [5]. SCLE lesions commonly lead to hypopigmentation or depigmentation and never lead to scarring. The systemic symptoms are mild like arthralgias and musculoskeletal complaints [5].
3.7.4 CCLE
This is also called discoid CLE characterized by erythematous discoid plaque that becomes hyperkeratotic and finally leads to atrophy and scarring and can lead to dyspigmentation; it mainly involves the face, ears, and neck but may be widespread, and there are no relation of sun exposure. This lesion can affect the mucosal membranes including the lips, mucosal surfaces of the mouth, nasal membranes, conjunctivae, and genital mucosa. CCLE has several types like hypertrophic/verrucous lupus erythematosus, lupus erythematosus tumidus, lupus panniculitis/profundus, chilblain lupus erythematosus, and DLE–lichen planus overlap [5].
3.8 Others
3.8.1 Photosensitivity
Macular rash present only after sun exposure may appear on the face, arms, or hands and persist for more than 1 day [6].
3.8.2 Discoid Rash
Erythematous patches with keratotic scaling over sun-exposed areas, plaque-like in character with follicular plugging and scarring [6] (Fig. 15.3).
3.8.3 Alopecia
Mainly affects the temporal regions or creates a patchy pattern of hair loss [7] (Fig. 15.4).
3.8.4 Oral Ulcer
It is an important manifestation of SLE; it occurs more than three times per year and is usually painless [7].
3.8.5 Systemic Sclerosis “Scleroderma”
Scleroderma is a term used to describe a thickened skin. It may affect the skin and subjacent tissues, or it may be associated with systemic involvement [8].
3.8.6 Raynaud Phenomenon
Changes of the color of the digits due to abnormal vasoconstriction of digital arteries and cutaneous arterioles due to a local defect in normal vascular responses, (pallor , cyanosis and then redness). It is exaggerated by cold temperatures or emotional stress [9] (Fig. 15.5)
3.9 Telangiectasia
It may develop anywhere within the body but mostly seen in perioral area, hands, and anterior chest. It’s small dilated blood vessels that locate beneath the dermis on skin (venule) (Fig. 15.6).
3.10 Sclerodactyly
It is a localized thickening and tightness of the skin of the fingers or toes. Sclerodactyly is commonly associated with atrophy of the underlying soft tissues. It is considered as a characteristic feature of scleroderma (Fig. 15.7).
3.11 Cutaneous Sclerosis
It is the formation of scar tissue in the skin or in tissues around joints (Fig. 15.8).
Note the tight and shiny appearance of skin.
3.12 Digital Ulcers
With scleroderma, repeated episodes of spasm of the fingers (Raynaud’s) can cause pitted fingertip scars, and in some people this results in fingertip ulcers [10].
3.13 Calcinosis Cutis
It is mostly asymptomatic and developed gradually, in which amorphous, insoluble calcium salt deposits in the skin and subcutaneous tissue [11]. It’s usually firm, multiple, whitish dermal papules, plaques, nodules, or subcutaneous nodules. The lesion spontaneously ulcerated, and it may be tender and may restrict joint mobility. In severe cases it may cause cutaneous gangrene due to vascular calcification which diminishes the pulse.
Hyperpigmentation and finger swelling are also considered as skin manifestations which occur in systemic sclerosis.
4 Psoriasis
4.1 Scales (Fig. 15.9)
4.1.1 Nail Involvement
Nail disease is more common in patients with psoriatic arthritis [12]. There is usually involvement of the nail matrix or nail bed. Nail abnormalities may include: beau lines, leukonychia, onycholysis, oil spots, subungual hyperkeratosis, splinter hemorrhages, spotted lunulae, transverse ridging, cracking of the free edge of the nail, and uniform nail pitting.
4.1.2 Erythroderma
Patients commonly present with generalized erythema, then after the onset of erythema 2–6 weeks, scaling appears usually from flexural area. Pruritus commonly results in excoriations. If it persist for weeks, hair may shed, nails may become ridged, thickened and it may shed. Inflammation and edema in periorbital skin may occur resulting in ectropion (Fig. 15.10).
4.1.3 Guttate Lesion
It is a clinical presentation that is characterized by a distinctive, acute eruption of small, droplike, 1–10 mm in diameter, salmon-pink papules, usually with a fine scale. It occurs primarily on the trunk and the proximal extremities; also it may have general distribution on the body [13] (Fig. 15.11).
4.1.4 Psoriatic Arthritis
Psoriatic arthritis is one of the seronegative spondyloarthropathies which include ankylosing spondylitis and reactive arthritis. The prevalence of psoriatic arthritis among individuals with psoriasis is ranging from 7 to 48% [14,15,16,17,18]. There are several patterns of joint involvement in psoriatic arthritis patients [19]:
-
Distal arthritis which involves distal interphalangeal (DIP) joints.
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Asymmetric oligoarthritis.
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Symmetric polyarthritis.
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Arthritis mutilans, characterized by deforming and destructive arthritis.
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Spondyloarthropathy which includes sacroiliitis and spondylitis.
4.2 Dermatomyositis (DM)
4.2.1 Gottron’s Papules
They are symmetrical erythematous eruptions which involve the extensor aspects of the metacarpophalangeal (MCP) and interphalangeal (IP) joints and may involve the skin between them; they may be associated with scale and ulcer if the eruption was prominent [20] (Fig. 15.12).
4.2.2 Heliotrope Eruption
Erythematous lesion occurs on the upper eyelids and may be associated with eyelid edema (Fig. 15.13).
4.3 Facial Erythema
This lesion can mimic the malar rash seen in SLE. To easily differentiate between both of them, look at the nasolabial fold; if it is involved, then the rash is mainly due to DM; however, if it is not involved, then the rash is mainly due to SLE (Fig. 15.14).
4.4 Photodistributed Poikiloderma
Poikiloderma consists of both hyperpigmentation and hypopigmentation; it always occurs in upper chest, the V of the neck, and upper back (shawl sign); it may come as macular (nonpalpable) or papular erythema if it happens in early stages of cutaneous disease. It is usually associated with pruritus, and this is the difference between DM and photo-exacerbated eruption of lupus erythematosus. If the patient presents with poikiloderma on the lateral aspects of the thighs, this is now called Holster sign (Fig. 15.15).
4.5 Periungual Abnormalities
These are characterized by erythematous lesion with vascular changes in the capillary nail beds which also may be associated with areas of dilatation and dropout and with periungual erythema [21].
4.6 Psoriasiform Changes in Scalp
The scalp lesion in DM is diffuse, associated with prominent scaling and poikilodermatous changes. It may be difficult to distinguish from seborrheic dermatitis and psoriasis. It happens usually as a result of severe burning, pruritus, or sleep disturbance.
4.7 Calcinosis Cutis
It is more common in juvenile DM than adult DM. It means deposition of calcium within the skin. It is associated with a delay in treatment with glucocorticoids and immunosuppressive therapy; this lesion can be seen in other diseases like systemic sclerosis and SLE but more common with DM [22, 23].
4.8 Reactive Arthritis
4.8.1 Circinate Balanitis
It is an asymptomatic genital lesion characterized by shallow ulcers in the penis [24].
4.8.2 Keratoderma
Hyperkeratotic skin rashes involve soles and palms [24] (Fig. 15.16).
4.9 Hepatitis C Virus (HCV)
4.9.1 Porphyria Cutanea Tarda
It is a skin lesion strongly associated with HCV and characterized by photosensitivity, bruising skin, fragility, facial hirsutism, and vesicles or bullae that can become hemorrhagic. It is a skin disease caused by a reduction of hepatic uroporphyrinogen decarboxylase activity [25].
4.9.2 Leukocytoclastic Vasculitis
This lesion is usually associated with palpable purpura and petechiae that usually involve the lower extremities and may happen in conjunction with essential mixed cryoglobulinemia; in skin biopsy, there is dermal blood vessel destruction associated with a neutrophilic infiltration in and around the vessel wall (Fig. 15.17) [26].
4.10 Lichen Planus
It involves mucus membranes, hair, and nails characterized by flat-topped, violaceous, pruritic papules with a generalized distribution. In skin biopsy, there is a dense lymphocytic infiltration in the upper dermis [27, 28] (Fig. 15.18).
4.11 Necrolytic Acral Erythema
This lesion is pruritic and characterized by sharply marginated, erythematous to hyperpigmented plaques with variable scale and erosion which involves the lower extremities (Fig. 15.19) [29].
4.12 Polyarteritis Nodosa
4.12.1 Livedo Reticularis
It is characterized by tenderness and it does not blanch with active pressure [30,31,32].
4.12.2 Ulcerations
It usually involves the lower extremities [30,31,32].
4.13 Digital Ischemia
It may be associated with splinter hemorrhages and gangrene [30,31,32].
5 Sarcoidosis
It is a granulomatous disease and defined as presence of non-caseating granulomas in different tissues and organs such as lymph nodes, eyes, joints, brain, kidneys, lung, and skin. The signs that appear with sarcoidosis are as follows.
5.1 Erythema Nodosum
It is the most common nonspecific lesion of sarcoidosis and characterized by inflammatory, tender, erythematous, subcutaneous plaques and nodules in the anterior tibial areas. The patient can present with low-grade fever, arthritis, and lower extremity edema (Fig. 15.20) [32].
5.2 Papular Sarcoidosis
It is the most common specific lesion characterized by numerous non-scaly, skin-colored, yellow-brown, red-brown, violaceous, or hypopigmented 1 to 10 mm papules, and the papules can demonstrate a slight central depression. The most common site is the face, with a predilection for the eyelids and nasolabial folds [33].
5.3 Nodular Sarcoidosis
Subcutaneous sarcoidosis or nodular sarcoidosis, all these terms describe the nodule arising from subcutaneous tissue [32]; it is one of the most common lesions in sarcoidosis, and it results from large collections of sarcoidal granulomas in the dermis or subcutaneous tissue characterized as asymptomatic or mildly tender, flesh-colored, erythematous, violaceous, and hyperpigmented. The upper extremities are the most common site of nodular sarcoidosis [34]. It can be single or multiple, and its size could be about 1 and 2 cm in diameter. The differential diagnosis of subcutaneous sarcoidosis includes lipomas, cysts, cutaneous manifestations of lymphoproliferative malignancies, subcutaneous granuloma annulare, foreign body, or granulomas [35, 36].
5.4 Maculopapular Sarcoidosis
This lesion is characterized by raised papules that are often around 1 mm in diameter, slightly tender, pruritic, slightly hyperpigmented patches, red, brown, or violaceous in color [37]; the most common sites are facial and eyelid areas, and it may involve mucous membranes, neck, trunk, or extremities [32].
5.5 Plaque Sarcoidosis
This lesion is characterized by oval or annular shaped, indurated, different color such as flesh-colored, erythematous or brown rash that may have scale at the end stage. The most common sites involved are the arms, shoulders, back, and buttocks; it has common features with psoriasis, lichen planus, discoid lupus, granuloma annulare, cutaneous T cell lymphoma, secondary syphilis, and Kaposi’s sarcoma [36].
5.6 Lupus Pernio
This lesion is characterized by erythematous, indurated papules, plaques, or nodules [38]; the most common sites involved are the face, nasal tip, alar rim, and cheeks, and it may involve ears and lips [39]. If this lesion is not treated, it will progress rapidly and increase in thickness, size, and induration. After the lesion is resolved, it will leave scar [37]. This lesion is associated more with extracutaneous manifestations such as respiratory tract involvement and lytic and cystic bone lesions [40].
5.7 Hypopigmented Sarcoidosis
It affects mostly dark-skinned persons of African descent, and the lesion is characterized by round to oval, hypopigmented, well-demarcated patches and may have raised plaques [33, 41].
5.8 Atrophic and Ulcerative Sarcoidosis
This lesion is a combined lesion meaning it is involved with atrophic and ulcerated lesions, which are characterized by depressed plaques not elevated [42]; this lesion is associated with other mucocutaneous manifestations of sarcoidosis. The ulcerative lesion is more common in women and black patients [43].
6 Rheumatic Fever
Acute rheumatic fever is a non-suppurative sequela that occurs after 2–3 weeks of group A streptococcus and pharyngitis. It mostly affects children aged 5 to 15 years. This disease is characterized by arthritis, carditis, chorea, erythema marginatum, and subcutaneous nodules. The damage to the cardiac valve is chronic and it may progress [44].
To make a diagnosis of rheumatic fever, there is a special criterion called Jones Criteria, which involves major and minor manifestations which are as follows.
The major manifestations:
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Arthritis.
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Carditis.
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Chorea.
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Erythema marginatum.
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Subcutaneous nodules.
The minor manifestations:
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Arthralgia.
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Fever.
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Elevated acute phase reactants (erythrocyte sedimentation rate [ESR], C-reactive protein [CRP]).
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Prolonged PR interval.
In this chapter we will talk only about the rheumatological and dermatological manifestations, which are as follows.
6.1 Arthritis
It is the early symptom of rheumatic fever. The classical history of arthritis involves migratory polyarthritis within days to a week. The meaning of migratory is “it affects the joint then migrates to the other joint”; the most common joints involved are knees, elbows, and wrists [36]; the patient will complain of limitation in his movement because of the severity of the joint pain. The inflammation of each joint lasts no more than 1 week and the signs of inflammation are usually present [45].
6.2 Erythema Marginatum
This lesion appears early in the course of the rheumatic fever characterized by an evanescent, pink or faintly red, non-pruritic rash; the outer edge is sharp and the inner is diffuse; it has continuous margins and sometimes has a ring shape. It usually affects the trunk and may affect the limbs, but it is unlikely to affect the face [46]. The course of this lesion is intermittent meaning that it appears, disappears, and then reappears in a matter of hours [47].
6.3 Subcutaneous Nodules
This lesion is characterized by symmetrical, firm, painless lesions ranging from a few millimeters to 2 cm in size, and the average number of nodules is about three to four, and it has non-inflamed skin above it. The nodules present over the bony surface or prominence or near tendons. This lesion appears 1 week after the disease and is associated with sever carditis lasting no more than 1 month. We can distinguish rheumatic fever nodules from rheumatic arthritis nodules as the rheumatic fever nodules are smaller and more short-lived than the nodules of rheumatoid arthritis and almost involve the olecranon, while rheumatoid nodules are usually found 3 to 4 cm distally; finally all of them involve the elbows [48].
7 Behçet’s Disease
Behçet’s disease is a complex, multi-systemic disease that involves the mucocutaneous, ocular, cardiovascular, renal, gastrointestinal, pulmonary, urologic, and central nervous systems, the joints, blood vessels, and lungs. Men are more commonly affected by this disease than women, and it is more common in the third decade of life, but it can occur at any age. Signs and symptoms of this disease may precede the onset of the mucosal membrane ulcerations by 6 months to 5 years, and prior to the onset of the disease, the patient experiences generalized and various symptoms.
In patients with Behçet’s disease, a variety of cutaneous changes appear on them [49].
7.1 Erythema Nodosum-like Lesion
It is red to violet and painful subcutaneous nodule. It occurs on the extremities especially the lower extremities; also it can present on the face, neck, and buttocks. It resolves spontaneously or it may ulcerate leaving a scar and hyperpigmentation area.
7.2 Acneiform Lesion
It may be more common in those with associated arthritis [50]. It consists of papules and pustules that are difficult to distinguish from ordinary acne [51].
7.3 Folliculitis-like Rash
It distributes on the back, face, neck, chest, and hairline of patients. It resembles acne vulgaris.
7.4 Papulopustular Eruptions
Pustular skin lesions are often not sterile and may contain Staphylococcus aureus and Prevotella spp. [52].
7.5 Erythema Multiforme-like Lesions
7.6 Superficial Thrombophlebitis
It is a migratory superficial thrombophlebitis of the skin. It may be associated with deep vein thrombosis that causes lower extremities edema.
7.7 Ulcers (Oral, Genital)
During physical exam:
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Oral ulcer: difficult to distinguish from common aphthae (Table 15.1).
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The most common sites are the tongue, lips, buccal mucosa, and gingiva; the tonsils, palate, and pharynx are less common sites. The interval between recurrences ranges from weeks to months.
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Genital ulcers: recurrent and painful, and it may cause scarring.
7.8 Pyoderma Gangrenosum
It is an ulcerative cutaneous condition starting from a small, red papule or pustule and then changing into an ulcerative lesion.
7.9 Positive Pathergy Reaction at Injection Site
Nonspecific inflammatory reaction to scratches and intradermal saline injection is a common and specific manifestation to these lesions.
7.10 Arthritis
During an exacerbation of disease, a non-erosive, asymmetrical arthritis occurs in about 50% of patients with this disease. It involves large and medium joints (wrist, knee, and ankle). Also for the patient with Behçet’s disease, experiencing myalgias and migratory arthralgias without overt arthritis is common. On the other hand, arthritis occurs in about 50% of patients with Behçet’s disease [53].
There are also genital, ocular, gastrointestinal, joint, and neurologic manifestations.
8 Inflammatory Bowel Disease
Inflammatory bowel disease (IBD) includes two major disorders, which are ulcerative colitis and Crohn’s disease. This group of diseases cause many extraintestinal manifestations including eye, skin, joint, renal, and urologic conditions. In this chapter we will talk about skin and the musculoskeletal manifestations of IBD. The most common skin lesions presenting with IBD are erythema nodosum and pyoderma gangrenosum and other less common lesions such as Sweet syndrome, necrotizing cutaneous vasculitis, and psoriasis.
8.1 Erythema Nodosum (EN)
This lesion is equally present in ulcerative colitis and Crohn’s disease, and it is characterized by raised, tender, red or violet subcutaneous nodules, which are around 1 to 5 cm in diameter. The most common sites involved are the extensor surfaces of the extremities, specifically over the anterior tibial area. The presence of erythema nodosum reflects the activity of the intestinal disease and usually disappears by management of intestinal manifestations. Also this lesion is diagnosed clinically, and if we take a biopsy, it will show focal panniculitis, which is rarely done [54].
8.2 Pyoderma Gangrenosum
This lesion is less common than EN, and it has a severe course because of its persistence, and it is an uncomfortable lesion preceded by trauma to the skin and initially appears as single or multiple erythematous papules or pustules [55]. The most common site involved is the legs, but it can appear at any site including abdomen and at the site of surgical scars or at the stoma after colectomy. It may form deep ulceration that contains purulent material by subsequent necrosis of the dermis, and usually the culture of the purulent material is sterile. Pyoderma gangrenosum reflects the activity of IBD disease, and it needs a course of high-dose glucocorticoids over several weeks of treatment [56].
8.3 Oral Ulcer
It is a common manifestation in patients with IBD, especially patients with Crohn’s disease.
8.4 Musculoskeletal Manifestations
The musculoskeletal manifestations of IBD are considered the most common extra-intestinal manifestation, and they include; non-destructive peripheral arthritis and axial arthritis, other less common musculoskeletal manifestations are osteoporosis, osteopenia, and osteonecrosis.
8.5 Arthritis
The joints that are involved are the spine, sacroiliac joints, and appendicular joints; there are two types of peripheral arthritis: type 1 is acute and remitting and type 2 is a chronic problem and causes frequent relapses; other joint pain can result from complications of IBD such as bacterial infection of the sacroiliac or peripheral joints or as adverse effects from chronic use of glucocorticoid such as osteonecrosis, and those complications must be distinguished from sterile inflammation [57].
9 Severe and Life-Threatening Conditions (Fig. 15.21)
10 Stevens-Johnson Syndrome (SJS) and Toxic Epidermal Necrolysis (TEN)
They are rare, acute immune complex medited hypersensitive and life that are nearly always drug-related. Allopurinol is the most common cause [58]. They are a consequence of extensive keratinocyte cell death that results in the separation of significant areas of skin at the dermal-epidermal junction, producing the appearance of scalded skin [59]. We can classify this disease simply into as follows:
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Stevens-Johnson syndrome (a minor form of toxic epidermal necrolysis): less than 10% body surface area (BSA) detachment.
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Overlapping Stevens-Johnson syndrome/toxic epidermal necrolysis: detachment of 10–30% of the BSA.
Toxic epidermal necrolysis: detachment of more than 30% of the BSA.
The initial symptoms of Stevens-Johnson syndrome and toxic epidermal necrolysis that precede cutaneous manifestations by 1 to 3 days are fever, productive cough with thick purulent sputum, pain on swallowing, headache, arthralgia, and malaise.
A patient with SJS and TEN may complain of a rash, which appears first on the trunk, spreading to the neck, face, and proximal upper extremities. The following points are characteristic of cutaneous lesions:
10.1 Rash
It first appears as macules and then develops into papules, vesicles, bullae, urticarial plaques, or confluent erythema (erythroderma) (Fig. 15.22).
10.2 Bullous Lesions
It appears as flaccid blisters and may rupture leaving denuded skin (Fig. 15.23).
10.3 Urticarial Lesions (Not Pruritic)
It may be edematous, erythematous to pale area involving the dermis and epidermis (Fig. 15.24).
10.4 Erythema
Erythema and erosions of the buccal, ocular, and genital mucosae are present in more than 90% of patients.
10.5 Palpable Purpura
10.6 Edema (Face, Tongue)
10.6.1 Sloughing of Skin
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Skin looks like wet cigarette paper.
-
Skin ulceration.
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Skin necrosis.
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Nikolsky sign: it should be sought by exerting tangential mechanical pressure with a finger on several erythematous zones and considered positive if dermal-epidermal cleavage is induced (Fig. 15.25).
11 Erythroderma Exfoliation
More than 90% of body surface areas are involved by generalized redness and scaling of the skin due to generalization of pre-existing dermatoses (such as psoriasis or atopic dermatitis), drug reactions, or cutaneous T-cell lymphoma (CTCL) [60]. The clinical features are as follows:
11.1 Erythema
11.1.1 Exfoliation and Scales (2–6 Days after Erythema)
There is variation in the size and the color of the scales. In acute phases, scales are usually large and crusted while in chronic states are smaller and drier. Occasionally, the cause of the erythroderma is suggested by the character of the scale:
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Fine scale in atopic dermatitis or dermatophytosis.
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Bran-like in seborrheic dermatitis.
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Crusted in pemphigus foliaceus.
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Exfoliative in drug reactions.
11.2 Pruritus
Approximately 90% of patients complain from it, so it is the most frequent complaint. Thickness of the skin and areas of lichenification are seen in one-third of cases due to itching.
11.3 Pain
Most patients complain of severe skin pain.
11.4 Dyspigmentation
Hyperpigmentation area (45%) observed more frequently than hypo- or depigmentation (20%).
11.5 Palmoplantar Keratoderma
Hyperkeratosis of the palms and soles. Approximately 30% of erythrodermic patients present with it.
11.6 Nail Changes
They are related to the underlying cause of erythroderma, for example, pit in psoriasis or horizontal ridging in dermatitis. Most often “shiny” nails are observed, but discoloration, brittleness, dullness, subungual hyperkeratosis, Beau’s lines, paronychia, and splinter hemorrhages can be seen.
11.7 Diffuse Non-scarring Alopecia
It appears in 20% of patients with chronic erythroderma.
11.8 Systemic Manifestation
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Generalized peripheral lymphadenopathy.
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Pedal or pretibial edema.
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Facial edema.
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Tachycardia.
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Splenomegaly is rarely seen and occurs most often in association with lymphoma.
11.9 Complications
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Multiple seborrheic keratosis.
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Cutaneous infection with Staphylococcus aureus.
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Bilateral ectropion.
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Purulent conjunctivitis.
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Risk of cardiac failure.
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Anemia.
12 Gonococcal Arthritis
Considered as the most common form of septic arthritis in the United States and caused by gram-negative diplococcus Neisseria gonorrhoeae. It is composed of two forms:
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Bacteremic form (arthritis-dermatitis syndrome).
-
Septic arthritis form (localized to the joint) [58]
Bacteremic form (arthritis-dermatitis syndrome)
-
Migratory arthralgias and arthritis:
It presents as:
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Polyarticular.
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Asymmetric.
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Upper extremities involvement more than lower extremities.
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The most commonly affected joints are wrists, elbows, knees, and ankles.
-
It may evolve into a septic arthritis.
-
-
Tenosynovitis:
An inflammation that involves the tendon and its sheath; it is almost always asymmetrical and commonly over the dorsum of the wrist and hands. Also, it can affect the ankle, knee, and metacarpophalangeal joints [60].
-
Dermatitis:
Around 40–70% of patients with bacteremic form are affected.
It presents as:
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Tiny maculopapular, pustular, or vesicular lesions on an erythematous base.
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Painless and non-pruritic lesions.
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The lesion’s center may become necrotic or hemorrhagic.
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The lesions may rarely resemble erythema nodosum or erythema multiforme [60].
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Other presentations may include:
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Fever, rarely higher than 39 °C.
-
Fitz-Hugh-Curtis syndrome (gonococcal perihepatitis).
-
Sepsis with Waterhouse-Friderichsen syndrome.
-
Gonococcal endocarditis (rare in the antibiotic era).
-
Gonococcal meningitis (very rare in the antibiotic era).
Septic arthritis form:
It presents as an acute inflammation to the joints with signs of:
-
Joint effusion.
-
Warmth.
-
Tenderness.
-
Reduced range of motion.
-
Marked erythema.
One form of complication is permanent joint damage. Other complications are pericarditis, perihepatitis, pyomyositis, glomerulonephritis, meningitis, endocarditis, and osteomyelitis [58].
Abbreviations
- RA:
-
Rheumatoid arthritis
- PND:
-
Paraneoplastic neurological disorders
- HCV:
-
Hepatitis C virus
- SLE:
-
Systemic lupus erythematosus
- ACLE:
-
Acute cutaneous lupus erythematosus
- SCLE:
-
Subacute cutaneous lupus erythematosus
- CCLE:
-
Chronic cutaneous lupus erythematosus
- DLE:
-
Discoid lupus erythematosus
- DIP:
-
Distal interphalangeal joint
- DM:
-
Dermatomyositis
- CTCL:
-
Cutaneous T-cell lymphoma
- ESR:
-
Erythrocyte sedimentation rate
- CRP:
-
C-reactive protein
- IBD:
-
Inflammatory bowel disease
- EN:
-
Erythema nodosum
- SJS:
-
Stevens-Johnson syndrome
- TEN:
-
Toxic epidermal necrolysis
- BSA:
-
Body surface area
References
Garcia-Patos V. Rheumatoid nodule. Semin Cutan Med Surg. 2007;26(2):100–7. https://doi.org/10.1016/j.sder.2007.02.007.
Sayah A, English JC 3rd. Rheumatoid arthritis: a review of the cutaneous manifestations. J Am Acad Dermatol. 2005;53(2):191–209; quiz 210-192. https://doi.org/10.1016/j.jaad.2004.07.023.
Turesson C, McClelland RL, Christianson T, Matteson E. Clustering of extraarticular manifestations in patients with rheumatoid arthritis. J Rheumatol. 2008;35:179–80.
Oien RF, Hakansson A, Hansen BU. Leg ulcers in patients with rheumatoid arthritis--a prospective study of aetiology, wound healing and pain reduction after pinch grafting. Rheumatology (Oxford). 2001;40(7):816–20.
Böhm M, Luger TA Skin in Rheumatic disease. In GS Firestein, RC Budd, SE Gabriel, IB Mcinnes & JR O'Dell (Eds.), Kelley's Textbook Of Rheumatology (9th ed.)
Callen JP. Systemic lupus erythematosus in patients with chronic cutaneous (discoid) lupus erythematosus. Clinical and laboratory findings in seventeen patients. J Am Acad Dermatol. 1985;12(2 Pt 1):278–88.
Healy E, Kieran E, Rogers S. Cutaneous lupus erythematosus--a study of clinical and laboratory prognostic factors in 65 patients. Ir J Med Sci. 1995;164(2):113–5.
LeRoy EC, Black C, Fleischmajer R, Jablonska S, Krieg T, Medsger TA Jr, et al. Scleroderma (systemic sclerosis): classification, subsets and pathogenesis. J Rheumatol. 1988;15(2):202–5.
Wigley FM. Clinical practice. Raynaud's phenomenon. N Engl J Med. 2002;347(13):1001–8. https://doi.org/10.1056/NEJMcp013013.
Reiter N, El-Shabrawi L, Leinweber B, Berghold A, Aberer E. Calcinosis cutis: part I. diagnostic pathway. J Am Acad Dermatol. 2011;65(1):1–12.; quiz 13-14. https://doi.org/10.1016/j.jaad.2010.08.038.
Klaassen KM, van de Kerkhof PC, Pasch MC. Nail psoriasis: a questionnaire-based survey. Br J Dermatol. 2013;169(2):314–9. https://doi.org/10.1111/bjd.12354.
Baker BS, Owles AV, Fry L. A possible role for vaccination in the treatment of psoriasis? G Ital Dermatol Venereol. 2008;143(2):105–17.
Gelfand JM, Gladman DD, Mease PJ, Smith N, Margolis DJ, Nijsten T, et al. Epidemiology of psoriatic arthritis in the population of the United States. J Am Acad Dermatol. 2005;53(4):573. https://doi.org/10.1016/j.jaad.2005.03.046.
Reich K, Kruger K, Mossner R, Augustin M. Epidemiology and clinical pattern of psoriatic arthritis in Germany: a prospective interdisciplinary epidemiological study of 1511 patients with plaque-type psoriasis. Br J Dermatol. 2009;160(5):1040–7. https://doi.org/10.1111/j.1365-2133.2008.09023.x.
Radtke MA, Reich K, Blome C, Rustenbach S, Augustin M. Prevalence and clinical features of psoriatic arthritis and joint complaints in 2009 patients with psoriasis: results of a German national survey. J Eur Acad Dermatol Venereol. 2009;23(6):683–91. https://doi.org/10.1111/j.1468-3083.2009.03159.x.
Ibrahim G, Waxman R, Helliwell PS. The prevalence of psoriatic arthritis in people with psoriasis. Arthritis Rheum. 2009;61(10):1373–8. https://doi.org/10.1002/art.24608.
Mease PJ, Gladman DD, Papp KA, Khraishi MM, Thaci D, Behrens F, et al. Prevalence of rheumatologist-diagnosed psoriatic arthritis in patients with psoriasis in European/North American dermatology clinics. J Am Acad Dermatol. 2013;69(5):729–35. https://doi.org/10.1016/j.jaad.2013.07.023.
Garg A, Gladman D. Recognizing psoriatic arthritis in the dermatology clinic. J Am Acad Dermatol. 2010;63(5):733–48; quiz 749-750. https://doi.org/10.1016/j.jaad.2010.02.061.
Dugan EM, Huber AM, Miller FW, Rider LG. Photoessay of the cutaneous manifestations of the idiopathic inflammatory myopathies. Dermatol Online J. 2009;15(2):1.
Smith RL, Sundberg J, Shamiyah E, Dyer A, Pachman LM. Skin involvement in juvenile dermatomyositis is associated with loss of end row nailfold capillary loops. J Rheumatol. 2004;31(8):1644–9.
Gunawardena H, Wedderburn LR, Chinoy H, Betteridge ZE, North J, Ollier WE, et al. Autoantibodies to a 140-kd protein in juvenile dermatomyositis are associated with calcinosis. Arthritis Rheum. 2009;60(6):1807–14. https://doi.org/10.1002/art.24547.
Ceribelli A, Fredi M, Taraborelli M, Cavazzana I, Franceschini F, Quinzanini M, et al. Anti-MJ/NXP-2 autoantibody specificity in a cohort of adult Italian patients with polymyositis/dermatomyositis. Arthritis Res Ther. 2012;14(2):R97. https://doi.org/10.1186/ar3822.
Lee LA, Werth VP The skin and rheumatic diseases. In GS Firestein, RC Budd, SE Gabriel, IB Mcinnes & JR O'Dell (Eds.), Kelley's Textbook Of Rheumatology (9th ed.).
Gisbert JP, Garcia-Buey L, Pajares JM, Moreno-Otero R. Prevalence of hepatitis C virus infection in porphyria cutanea tarda: systematic review and meta-analysis. J Hepatol. 2003;39(4):620–7.
David WS, Peine C, Schlesinger P, Smith SA. Nonsystemic vasculitic mononeuropathy multiplex, cryoglobulinemia, and hepatitis C. Muscle Nerve. 1996;19(12):1596–602. https://doi.org/10.1002/(SICI)1097-4598(199612)19:12<1596::AID-MUS9>3.0.CO;2-5.
Pilli M, Penna A, Zerbini A, Vescovi P, Manfredi M, Negro F, et al. Oral lichen planus pathogenesis: a role for the HCV-specific cellular immune response. Hepatology. 2002;36(6):1446–52. https://doi.org/10.1053/jhep.2002.37199.
Protzer U, Ochsendorf FR, Leopolder-Ochsendorf A, Holtermuller KH. Exacerbation of lichen planus during interferon alfa-2a therapy for chronic active hepatitis C. Gastroenterology. 1993;104(3):903–5.
Abdallah MA, Ghozzi MY, Monib HA, Hafez AM, Hiatt KM, Smoller BR, Horn TD. Necrolytic acral erythema: a cutaneous sign of hepatitis C virus infection. J Am Acad Dermatol. 2005;53(2):247–51. https://doi.org/10.1016/j.jaad.2005.04.049.
Pagnoux C, Seror R, Henegar C, Mahr A, Cohen P, Le Guern V, et al. Clinical features and outcomes in 348 patients with polyarteritis nodosa: a systematic retrospective study of patients diagnosed between 1963 and 2005 and entered into the French Vasculitis study group database. Arthritis Rheum. 2010;62(2):616–26. https://doi.org/10.1002/art.27240.
Gibson LE, Su WP. Cutaneous vasculitis. Rheum Dis Clin N Am. 1995;21(4):1097–113.
Karlsberg PL, Lee WM, Casey DL, Cockerell CJ, Cruz PD Jr. Cutaneous vasculitis and rheumatoid factor positivity as presenting signs of hepatitis C virus-induced mixed cryoglobulinemia. Arch Dermatol. 1995;131(10):1119–23.
Yanardag H, Pamuk ON, Karayel T. Cutaneous involvement in sarcoidosis: analysis of the features in 170 patients. Respir Med. 2003;97(8):978–82.
Elgart ML. Cutaneous sarcoidosis: definitions and types of lesions. Clin Dermatol. 1986;4(4):35–45.
Ben Jennet S, Benmously R, Chaabane S, Fenniche S, Marrak H, Mohammed Z, Mokhtar I. Cutaneous sarcoidosis through a hospital series of 28 cases. Tunis Med. 2008;86(5):447–50.
Ahmed I, Harshad SR. Subcutaneous sarcoidosis: is it a specific subset of cutaneous sarcoidosis frequently associated with systemic disease? J Am Acad Dermatol. 2006;54(1):55–60. https://doi.org/10.1016/j.jaad.2005.10.001.
Lodha S, Sanchez M, Prystowsky S. Sarcoidosis of the skin: a review for the pulmonologist. Chest. 2009;136(2):583–96. https://doi.org/10.1378/chest.08-1527.
Mangas C, Fernandez-Figueras MT, Fite E, Fernandez-Chico N, Sabat M, Ferrandiz C. Clinical spectrum and histological analysis of 32 cases of specific cutaneous sarcoidosis. J Cutan Pathol. 2006;33(12):772–7. https://doi.org/10.1111/j.1600-0560.2006.00563.x.
Veien NK, Stahl D, Brodthagen H. Cutaneous sarcoidosis in Caucasians. J Am Acad Dermatol. 1987;16(3 Pt 1):534–40.
Mana J, Marcoval J, Graells J, Salazar A, Peyri J, Pujol R. Cutaneous involvement in sarcoidosis. Relationship to systemic disease. Arch Dermatol. 1997;133(7):882–8.
Jorizzo JL, Koufman JA, Thompson JN, White WL, Shar GG, Schreiner DJ. Sarcoidosis of the upper respiratory tract in patients with nasal rim lesions: a pilot study. J Am Acad Dermatol. 1990;22(3):439–43.
Terunuma A, Watabe A, Kato T, Tagami H. Coexistence of vitiligo and sarcoidosis in a patient with circulating autoantibodies. Int J Dermatol. 2000;39:551–3.
Albertini JG, Tyler W, Miller OF. Ulcerative sarcoidosis. Case report and review of the literature. Arch Dermatol. 1997;133(2):215–9.
Yoo SS, Mimouni D, Nikolskaia OV, Kouba DJ, Sauder DN, Nousari CH. Clinicopathologic features of ulcerative-atrophic sarcoidosis. Int J Dermatol. 2004;43(2):108–12.
Guidelines for the diagnosis of rheumatic fever. Jones Criteria. Update. Special writing Group of the Committee on rheumatic fever, endocarditis, and Kawasaki disease of the council on cardiovascular disease in the young of the American Heart Association. (1992). JAMA. 1992;268(15):2069–73.
Wallace MR, Garst PD, Papadimos TJ, Oldfield EC 3rd. The return of acute rheumatic fever in young adults. JAMA. 1989;262(18):2557–61.
Burke JB. Erythema marginatum. Arch Dis Child. 1955;30(152):359–65.
Perry CB. Erythema marginatum (rheumaticum). Arch Dis Child. 1937;12(70):233–8.
Baldwin JS, Kerr JM, Kuttner AG, Doyle EF. Observations on rheumatic nodules over a 30-year period. J Pediatr. 1960;56:465–70.
Demirkesen C, Tuzuner N, Mat C, Senocak M, Buyukbabani N, Tuzun Y, Yazici H. Clinicopathologic evaluation of nodular cutaneous lesions of Behcet syndrome. Am J Clin Pathol. 2001;116(3):341–6. https://doi.org/10.1309/gcth-0060-55k8-xctt.
Diri E, Mat C, Hamuryudan V, Yurdakul S, Hizli N, Yazici H. Papulopustular skin lesions are seen more frequently in patients with Behcet's syndrome who have arthritis: a controlled and masked study. Ann Rheum Dis. 2001;60(11):1074–6.
Tunc R, Keyman E, Melikoglu M, Fresko I, Yazici H. Target organ associations in Turkish patients with Behcet's disease: a cross sectional study by exploratory factor analysis. J Rheumatol. 2002;29(11):2393–6.
Hatemi G, Bahar H, Uysal S, Mat C, Gogus F, Masatlioglu S, et al. The pustular skin lesions in Behcet's syndrome are not sterile. Ann Rheum Dis. 2004;63(11):1450–2. https://doi.org/10.1136/ard.2003.017467.
Kim HA, Choi KW, Song YW. Arthropathy in Behcet's disease. Scand J Rheumatol. 1997;26(2):125–9.
Farhi D, Cosnes J, Zizi N, Chosidow O, Seksik P, Beaugerie L, et al. Significance of erythema nodosum and pyoderma gangrenosum in inflammatory bowel diseases: a cohort study of 2402 patients. Medicine (Baltimore). 2008;87(5):281–93. https://doi.org/10.1097/MD.0b013e318187cc9c.
Powell FC, Schroeter AL, Su WP, Perry HO. Pyoderma gangrenosum: a review of 86 patients. Q J Med. 1985;55(217):173–86.
Keltz M, Lebwohl M, Bishop S. Peristomal pyoderma gangrenosum. J Am Acad Dermatol. 1992;27(2 Pt 2):360–4.
Wordsworth P. Arthritis and inflammatory bowel disease. Curr Rheumatol Rep. 2000;2(2):87–8.
Halevy S, Ghislain PD, Mockenhaupt M, Fagot JP, Bouwes Bavinck JN, Sidoroff A, et al. Allopurinol is the most common cause of Stevens-Johnson syndrome and toxic epidermal necrolysis in Europe and Israel. J Am Acad Dermatol. 2008;58(1):25–32. https://doi.org/10.1016/j.jaad.2007.08.036.
Sterry W, Steinhoff M. Papilosquamous and eczematous dermatoses. In: Bolognia JL, Jorizzo JL, Schaffer JV, editors. Dermatology. 3rd ed.
French IE, Prins C. Urticaria, erythema and purpuras. In: Bolognia JL, Jorizzo JL, Schaffer JV, editors. Dermatology. 3rd ed.
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Habibullah, T., Habibullah, A., Simsim, R. (2021). Skin Manifestations of Rheumatological Diseases. In: Almoallim, H., Cheikh, M. (eds) Skills in Rheumatology . Springer, Singapore. https://doi.org/10.1007/978-981-15-8323-0_15
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