Dermatology Flashcards

Question 1

Q

Define basal cell carcinoma.

Answer

A

The commonest form of skin malignancy.

= rodent ulcer

Question 2

Q

Explain the aetiology / risk factors of basal cell carcinoma.

Answer

A

Prolonged sun exposure or UV radiation
Photosensitizing pitch
Tar
Arsenic

Associated with abnormalities of the patched / hedgehog intracellular signaling cascade as seen in Gorlin’s Syndrome (naevoid basal cell carcinoma syndrome).

Question 3

Q

Summarise the epidemiology of basal cell carcinoma.

Answer

A

Common in those with fair skin and areas of high sunlight exposure, elderly, rare before 40 years

Lifetime risk in Caucasians = 1:3

Question 4

Q

Recognize the presenting symptoms of basal cell carcinoma.

Answer

A

A chronic slowly progressive skin lesion usually on the face but also on the scalp, ears or trunk.

Question 5

Q

Recognize the signs of basal cell carcinoma on physical examination.

Answer

A

Nodulo-Ulceractive:

Small glistening translucent skin over a coloured papule
Slowly enlarged (early)
Central ulcer with raised pearly edges
Fine telangiectatic vessels run over the tumour surface
Cystic changes in larger, more protuberant lesions

Morphoeic:

Expanding
Yellow / white waxy plaque
Ill-defined edge - more aggressive

Superficial:

Most often on trunk
Multiple pink / brown scaly plaques with a fine whipcord edge expanding slowly
Can grow to more than 10cm in diameter

Pigmented:
- Specks of brown or black pigment

Question 6

Q

Identify appropriate investigations for basal cell carcinoma and interpret the results.

Answer

A

Biopsy rarely necessary - diagnosis based on clinical suspicion.

Question 7

Q

Define burns injury.

Answer

A

Predominantly to the skin and superficial tissues, caused by heat from hot liquids, flame, or contact with heated objects, electrical current or chemicals.

Question 8

Q

Explain the aetiology / risk factors of burns injury.

Answer

A

Severity assess by burn size (% total body surface area) and depth (1st to 4th degree)

Risk Factors:

Young children
Age > 60 years
Male sex

Question 9

Q

Summarise the epidemiology of burns injury.

Answer

A

Very common injuries

Question 10

Q

Recognize the presenting symptoms of burns injury.

Answer

A

Dry and painful burns
Wet and painful burns
Dry and insensate burns

Question 11

Q

Recognize the signs of burns injury on physical examination.

Answer

A

Erythema
Clouded cornea
Cellulitis
Burns affecting subcutaneous tissue, tendon or bone

Question 12

Q

Identify appropriate investigations for burns injury and interpret the results.

Answer

A

FBC - low haematocrit, hypovolaemia, neutropenia, thrombocytopenia
Metabolic panel - high urea, creatinine, glucose, hyponatraemia, hypokalaemia
Carboxyhaemoglobin - high levels in inhalation injury
Arterial blood gas - metabolic acidosis in inhalation injury
Fluorescein staining - damaged corneal epithelial cells in corneal burns
CT scan of head and spine - brain injury, fracture in head or spine trauma
Wound biopsy culture - positive for the causative organism in wound infection sepsis
Wound histology - show wound infection

Question 13

Q

Define cellulitis and erysipelas.

Answer

A

Cellulitis - an acute spreading infection of the skin with visually indistinct borders that principally involves the dermis and subcutaneous tissue, characterised by redness, swelling, heat and tenderness and usually occurs in an extremity.

Erysipelas - a distinct form of superficial cellulitis with notable lymphatic involvement, that is raised and sharply demarcated from uninvolved skin.

Question 14

Q

Explain the aetiology / risk factors of cellulitis and erysipelas.

Answer

A

Often results from penetrating injury (e.g. IV cannulation), local lesions (e.g. insect bites, sebaceous cysts, surgery) or fissuring (e.g. in anal fissured, toe web spaces), which allows pathogenic bacteria to enter the skin.

In rare cases of septicaemia, it can arise spontaneously from blood-borne sources.

Most common organisms: Streptococcus pyogenes, Staphylococcus aureus. (MRSA not uncommon)

If occuring in orbit, Haemophilus influenzae is most common cause, arising from adjacent sinuses.

Risk Factors:

Diabetes
Venous insufficiency
Eczema
Oedema
Lymphoedema

Question 15

Q

Summarise the epidemiology of cellulitis and erysipelas.

Answer

A

Very common.

Main risk factors - skin break poor hygiene, poor vascularization of tissue (e.g. DM)

Question 16

Q

Recognise the presenting symptoms of cellulitis and erysipelas.

Answer

A

History of cut, scratch or injury.

Periorbital:
- Painful swollen red skin around eye

Orbital cellulitis:

Painful or limited eye movements
Visual impairment

Question 17

Q

Recognize the signs of cellulitis and erysipelas on physical examination.

Answer

A

Cellulitis - acute onset of red, painful, hot, swollen skin

Erysipelas - well-demarcated, bright-red raised skin

Lesion:

Erythema
Oedema
Warm tender indistinct margins
Pyrexia (may indicate systemic spread)
Orange-peel appearance
Bistering & bleeding

Exclude Abscess:

Test for fluid thrill or fluctuation
Aspirate if pus suspected

Periorbital:

Swollen eyelids
Conjunctival injection

Orbital Cellulitis:

Proptsis - protrusion of the eyeball
Impaired acuity and eye movement
Test for relative afferent pupillary defect, visual acuity and colour vision (to monitor optic nerve function)

Question 18

Q

Identify appropriate investigations for cellulitis and erysipelas and interpret the results.

Answer

A

Bloods

WCC / CRP / ESR
U&E
Blood culture

Discharge

Culture & sensitivity
Skin swab and biopsy

Aspiration
- Often non-purulent, not usually necessary

CT/MRI Scan
- When orbital cellulitis is suspected - to assess the posterior spread of infection

Question 19

Q

Generate a management plan for cellulitis and erysipelas.

Answer

A

Medical:

Oral penicillins - e.g. flucloxacillin, benzylpenicillin, coamoxiclav (community)
Tetracyclines (community)
Hospital - treat empirically using local microbiological guidelines but change depending on sensitivity of any cultured organisms
IV use may be necessary

Surgical
- Orbital decompression if orbital cellulitis (emergency)

Abscess
- Can be aspirated, incised and drained or excised completely

Question 20

Q

Identify the possible complications of cellulitis and erysipelas and its management.

Answer

A

Sloughing of overlying skin
Localised tissue damage
Orbital cellulitis - permanent vision loss, spread to brain, abscess formation, meningitis, carvenous sinus thrombosis

Question 21

Q

Summarise the prognosis for patients with cellulitis and erysipelas.

Answer

A

Good with treatment

Question 22

Q

Define eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic).

Answer

A

A pruritic papulovesicular skin reaction to endogenous or exogenous agents.

Discoid = Nummular

Dyshidrotic = Pompholyx

Herpeticum - a disseminated viral infection characterised by fever and clusters of itchy blisters or punched-out erosions (complication of atopic eczema)

Question 23

Q

Explain the aetiology / risk factors of eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic).

Answer

A

Numerous varieties caused by a diversity of triggers.

Exogenous:

Irritant - prolonged contact with a cell-damaging irritant (e.g. ammonia in nappy rash)
Contact - Type IV Delayed Hypersensitivity reaction to allergen (e.g. nickel, chromate, perfumes, latex, plants)
Phototoxic

Endogenous:

Atopic
Seborrhoeic - Pityrosporum yeast
Pomphloyx (dyshidrotic)
Varicose - increased venous pressure in lower limbs
Lichen simplex

Atopic:

Impaired epidermal barrier function due to intrinsic structural and functional skin abnormalities (predominant model)
Immune function disorder in which Langerhans cells, T-cells and immune effector cells modulate an inflammatory response to environmental factors

Lichen Simplex:

Thickening of skin secondary to a cycle of itch, scratch, itch
Characterised by well-demarcated hyperpigmented lichenified plaques

Question 24

Q

Summarise the epidemiology of eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic).

Answer

A

Contact - prevalence 4%

Atopic - onset in 1st year of life, childhood incidence 10-20%

Question 25

Q

Recognise the presenting symptoms of eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic).

Answer

A

Itching
Heat
Tenderness
Redness
Weeping
Crusting
Enquire into occupational exposures or irritants used at home (e.g. bleach)
Enquire into family / personal history of atopy (e.g. asthma, hay fever, rhinitis)

Question 26

Q

Recognise the signs of eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic) on physical examination.

Answer

A

Acute

Poorly demarcated erythematous oedematous dry scaling patches
Papules
Vesicles with exudation and crusting
Excoriation marks

Chronic

Thickened epidermis
Skin lichenification
Fissures
Change in pigmentation

Contact and Irritant:

Eczema reaction occurs where irritant / allergen comes into contact with skin
Autosensitization (spread to other sites)

Atopic:
- Face and flexures

Seborrhoeic:

Yellow greasy scales on erythematous plaques
Nasolabial folds, eyebrows, scalp, presternal area

Pompholyx (Dyshidrotic):
- Acute and often recurrent painful vesiculobullous eruption on palms and soles

Varicose:

Excema of lower legs
Associated with marked varicose veins

Nummular (Discoid) :
- Coin shaped, on legs and trunks

Asteatotic:

Dry
Crazy paring pattern

Question 27

Q

Identify appropriate investigations for eczema (including atopic, contact, discoid, dyshidrotic, herpeticum, seborrhoeic) and interpret the results.

Answer

A

Contact:

Skin patch testing - disc conatining postulated allergen is diluted and applied to back for 48h
Positive if allergen induces a red raised lesion

Atopic:

Laboratory testing not routinely used- including IgE levels
Swab for infected lesions (bacteria, fungi, viruses)

Question 28

Q

Define epidermoid and pilar cysts (sebaceous cysts).

Answer

A

A closed sac found under the skin, usually on the trunk, neck or face. They are filled with cheese-like matter and usually are painless.

Epidermoid cyst - a cyst where the cyst sac forms from cells that normally occur on the top layer of the skin (the epidermis).

Pilar cyst - a cyst where the cyst sac forms from cells similar to those that are in the bottom of the hair follicles (where hairs grow from).

Question 29

Q

Explain the aetiology / risk factors of epidermoid and pilar cysts (sebaceous cysts).

Answer

A

Risk Factors:

Hereditary tendency to form cysts - e.g. Gardner Syndrome, Gorlin Syndrome
High levels of testosterone
Male gender
Skin trauma
Swollen hair follicles

Question 30

Q

Summarise the epidemiology of epidermoid and pilar cysts (sebaceous cysts).

Answer

A

Epidermoid - most common cutaneous cysts, 3-4th decades of life, rare before puberty, M:F 2:1

Question 31

Q

Recognise the presenting symptoms of epidermoid and pilar cysts (sebaceous cysts).

Answer

A

Small, round bump under the skin, usually on the face, neck or trunk
Tiny blackhead plugging the central opening of the cyst
Thick, yellow, smelly material that sometimes drains from the cyst
Redness, swelling and tenderness in the area, if inflamed or infected

History:

How long has it been there?
Does it hurt?
Any other symptoms, e.g. itch?
Any other lumps?
Is it getting bigger?
Ever been abroad?
Otherwise well?

Question 32

Q

Recognise the signs of epidermoid and pilar cysts (sebaceous cysts) on physical examination.

Answer

A

Appear as firm, round, mobile subcutaneous nodules of varying size.

Common on face, scalp, neck and trunk.

Characteristic central punctum.

Infection common, foul pus exits through the punctum.

Question 33

Q

Identify appropriate investigations for epidermoid and pilar cysts (sebaceous cysts) and interpret the results.

Answer

A

Examination of the skin
Biopsy - rule out other skin growths
Skin culture - determine type of infection

Question 34

Q

Define erythema multiforme.

Answer

A

An acute hypersensitivity reaction of the skin and mucous membranes.

Stevens-Johnson Syndrome - severe form with bullous lesions and necrotic ulcers.

Question 35

Q

Explain the aetiology / risk factors of erythema multiforme.

Answer

A

Degeneration of basal epidermal cells and development of vesicles between the cells and the underlying basement membrane.

Lymphocytic infiltrate is seen around the blood vessels, and at the dermal-epidermal junction.

Immune complex deposition is variable and non-specific.

Precipitating factor only identified in 50% of cases.

Drugs:

Sulphonamides
Penicillin
Phenytoin
Barbiturates

Infection:

Viral - HSV, EBV, coxsackie, adenovirus, ORF
Bacterial - Mycoplasma pneumoniae, Chlamydiae
Fungal - Histoplasmosis

Inflammatory:

Rheumatoid arthritis
SLE
Sarcoidosis
Ulcerative colitis
Systemic vasculitis

Malignancy:

Lymphomas
Leukaemia
Myeloma

Radiotherapy

Question 36

Q

Summarise the epidemiology of erythema multiforme.

Answer

A

Any age group

M:F 2:1

Question 37

Q

Recognize the presenting symptoms of erythema multiforme.

Answer

A

Non-specfic prodromal symptoms of URTI
Sudeen appearance of itching, burning, painful skin lesion
May fade, leaving behind pigmentation

Question 38

Q

Recognize the signs of erythema multiforme on physical examination.

Answer

A

Classic target (bulls eye) lesions
Rim of erythema surrounding a paler area
Vesicles / bullae
Urticarial plaques
Symmetrical
Distributed over arms, legs, palms, soles, extensor surface

Stevens-Johnson Syndrome

Affecting > 2 mucous membranes - conjunctiva, cornea, lips (haemorrhagic crusts), mouth, genitalia
Systemic symptoms - sore throat, cough, fever, headache, myalgia, arthralgia, D&V
Shock - hypotension, tachycardia

Question 39

Q

Identify appropriate investigations for erythema multiforme and interpret the results.

Answer

A

Usually unnecessary as erythema multiforme and Stevens-Johnson Syndrome are clinical diagnoses.

Blood:

High WCC, eosinophils, ESR, CRP
Throat swab
Serology
Low albumin - in extensive exudation
High urea - due to catabolic state and dehydration
Autoantibodies

Imaging
- CXR - to exclude sarcoidosis and atypical pneumonias

Skin Biopsy
- Histology and direct immunofluorescence may be indicated in cases of diagnostic doubt

Question 40

Q

Define erythema nodosum.

Answer

A

Panniculitis (inflammation of the subcutaneous fat tissue) presenting as red or violet subcutaneous nodules.

Question 41

Q

Explain the aetiology / risk factors of erythema nodosum.

Answer

A

Delayed hypersensitivity reaction to antigens associated with various infectious agents, drugs and other diseases.

Infection:

Bacterial - Streptococcus, TB, Yersinia, rickettsia, Chlamydia, leprosy
Viral - EBV
Fungal - histoplasmosis, blastomycosis, coccidioidomycosis
Protozoal - toxoplasmosis

Systemic Disease:

Sarcoidosis
IBD
Behcet’s disease

Malignancy:

Leukaemia
Hodgkin’s disease

Drugs

Sulphonamides
Penicillin
Oral contraceptive pills

Pregnancy

Question 42

Q

Summarise the epidemiology of erythema nodosum.

Answer

A

25% of cases have no underlying cause.
Usually young adults.
M:F 3:1

Question 43

Q

Recognize the presenting symptoms of erythema nodosum.

Answer

A

Tender red or violet nodules
Bilaterally
Shins, thighs, forearms
Fatigue
Fever
Anorexia
Weight loss
Arthralgia
Symptoms of underlying aetiology

Question 44

Q

Recognise the signs of erythema nodosum on physical examination.

Answer

A

Crops of red or violet dome-shaped nodules
Present on both shins, thighs, forearms
Tender to palpation
Low-grade pyrexia
Tender joints, painful on movement
Signs of underlying aetiology

Question 45

Q

Identify appropriate investigations for erythema nodosum and interpret the results.

Answer

A

Determine underlying aetiology.

Bloods

Anti-streptolysin-O titre at diagnosis and 2-4 weeks later to assess for antecedent streptococcal infection
FBC
U&E
CRP
ESR
LFTs
Serum ACE - high in sarcoidosis

Throat Swab
- Culture

Mantoux / Heaf Skin Testing
- For TB

CXR
- To look for hilar adenopathy or other evidence of pulmonary sarcoidosis, TB and fungal infections

Question 46

Q

Define herpes simplex virus.

Answer

A

Includes HSV1 and HSV2.

Question 47

Q

Explain the aetiology / risk factors of herpes simplex virus.

Answer

A

Alpha-herpes virus with double-stranded deoxyribonucleic acid (dsDNA). Transmitted via close contact with an individual shedding the virus (e.g. kissing, sexual intercourse).

Multiply in epithelial cells of mucosal surface.

Produces vesicles or ulcers.

Lifelong latent infection when virus enters sensory neurons at infection site.

Can then reactivate, replicate and infect surrounding tissue - occurs in response to physical, emotional stresses or immunosuppression.

Disseminated infection if impaired T-cell immunity - e.g. pneumonitis, hepatitis, colitis

Risk Factors:

HIV infection
Immunosuppressive medications
High-risk sexual behaviour
Female sex
Black race
Increasing age
Lack of condom use

Question 48

Q

Summarise the epidemiology of herpes simplex virus.

Answer

A

HSV1 - infection in 2/3 of world’s population (approx 3.7 billion <50 years)

HSV2 - infection in 11% of world’s population ( approx 400 million)

90% adults seropositive for HSV1 by 30 years.
35% adults >60 years seropositive for HSV2.
1/3rd population recurrent HSV infections.

Question 49

Q

Recognise the presenting symptoms of herpes simplex virus.

Answer

A

HSV1 Primary Infection:

Asymptomatic
Pharyngitis
Gingivostomatitis - may make eating very painful
Herpetic whitlow - inoculation of virus into a finger

Recurrent infection / reactivation:

Prodrome (6h) peri-oral tingling and burning
Vesicles appear (48h), ulcerate and crust over
Complete healing 8-10 days

HSV2

Very painful blisters and rash in genital, perigenital and anal area
Dysuria
Fever
Malaise

HSV Keratoconjunctivitis:

Epiphoria - watering eyes
Photophobia

Question 50

Q

Recognise the signs of herpes simplex virus on physical examination.

Answer

A

Primary Infection:

Subclinical or sensory nerve prodrome (tingling)
Vesicles
Shallow ulcers

Systemic Symptoms:

Fever
Malaise
Tender cervical lymphadenopathy
Heals 8-12 days

Reactivation:
- Usually less severe unless immunosuppressed

Herpes Labialis:
- Cold sore lesion at lip border, predominantly HSV1

Genital Herpes:
- Predominantly HSV2

Gingivostomatitis:

Fever
Sore throat
Tender oropharyngeal vesicles
Yellow slough filled ulcers

Keratoconjunctivitis:

Corneal dendritic ulcers
Avoid steroids

Herpetic Whitlow:
- Painful vesicles on distal phalanx due to inoculation through a break in the skin

Herpes Encephalitis:

Most common treatable viral encephalitis
Transfer of virus from peripheral site to brain via neuronal transmission
Prodrome - fever, malaise, headache, nausea
Encephalopathy - general/ focal signs of cerebral dysfunction including psychiatric symptoms, seizure, focal neurology (temporal involvement in 60%), memory loss (HSV1 in immunocompetent patients)

Question 51

Q

Identify appropriate investigations for herpes simplex virus and interpret the results.

Answer

A

Clinical diagnosis
Confirmation required in encephalitis, keratoconjunctivitis or immunosuppression
Viral PCR of CSF, swab or vesicle scraping
Culture
Immunofluorescence
Serology

Question 52

Q

Define lipoma.

Answer

A

Slow growing, benign, mesenchymal tumours that form well-circumscribed, lobulated lesions composed of adipocytes.

Question 53

Q

Explain the aetiology / risk factors of lipomas.

Answer

A

Demarcated from surrounding fat by a thin, fibrous capsule
50% soft-tissue neoplasms
Encountered by primary care physicians, surgeons and pathologists
Usually arise in subcutaneous tissues
Can occur in any area of the body, most frequently trunk and proximal limbs
No malignant potential
DD - liposarcomas

Risk Factors:

Genetic predisposition
Trauma
Heavy alcohol consumption

Question 54

Q

Summarise the epidemiology of lipomas.

Answer

A

1% prevalence.
Incidence of 2.1 per 1000 per year.
5% of patients present with multiple lipomas.

Question 55

Q

Recognise the presenting symptoms of lipomas.

Answer

A

Soft, mobile, superficial cutaneous mass <5cm
Painless
Gastrointestinal obstruction
GI bleeding
Abdominal mass
Muscle weakness
Paraesthesia

Question 56

Q

Recognise the signs of a lipoma on physical examination.

Answer

A

Soft, mobile, superficial cutaneous mass <5cm
Painless
Gastrointestinal obstruction
GI bleeding
Abdominal mass
Muscle weakness
Paraesthesia - burning or prickling sensation that is usually felt on hands, arms, legs or feet

Question 57

Q

Identify appropriate investigations for a lipoma and interpret the results.

Answer

A

MRI if lesion >3cm and deep to the superficial fascia
CT
USS
Core needle biopsy
Incisional biopsy
Excisional biopsy
UGI contrast study - shows submucosal mass with no invasion of surroudning muscle layers or with evidence of mucosal involvement

Question 58

Q

Define melanoma and melanocytic lesions.

Answer

A

Malignancy arising from neoplastic transformation of melanocytes, the pigment-forming cells of the skin. The leading cause of death from skin disease.

Question 59

Q

Explain the aetiology /risk factors of melanoma and melanocytic lesions.

Answer

A

DNA damage in melanocytes caused by UV radiation results in neoplastic transformation.

50% arise in pre-existing naevi, 50% in previously normal skin.

4 Histopathological Types:

1) Superficial spreading (70%)
- Typically arises in a pre-existing naevus
- Expands in radial fashion before vertical growth phrase

2) Nodular (15%)
- Arises de novo
- Agressive
- No radial growth phrase

3) Lentigo Maligna (10%)
- More common in elderly with sun damage
- Large flat lesions
- Follow an indolent growth course
- Usually on the face

4) Acral Lentiginious (5%)
- Arise on palms, soles and subungual areas
- Most common type in non-white populations

Question 60

Q

Summarise the epidemiology of melanoma and melanocytic lesions.

Answer

A

Steadily increasing incidence
6000 per year diagnosed in the UK
Lifetime risk 1 in 80 in US
Whte races x20 risk to non-white races

Question 61

Q

Recognize the presenting symptoms of melanoma and melanocytic lesions.

Answer

A

Change in size, shape or colour of a pigmented skin lesion, redness, bleeding, crusting, ulceration

Question 62

Q

Recognise the signs of melanoma and melanocytic lesions on physical examination.

Answer

A

ABCDE

A = Asymmetry 
B = Border irregularity / bleeding 
C = Colour variation 
D = Diameter >6cm 
E = Elevation

Question 63

Q

Identify appropriate investigations for melanoma and melanocytic lesions and interpret the results.

Answer

A

Excisional Biopsy
Lymphoscintigraphy
Sentinel Lymph Node Biopsy
Staging
Blood

Excisional Biopsy
- For histological diagnosis and determination of Clark’s Levels or Breslow Thickness

Lymphoscintigraphy

Radioactive compound injected around lesion
Dynamic images taken over the course of 30 mins to trace the lymph drainage and the sentinel nodes

Sentinel Lymph Node Biopsy
- Dissected and histologically examined for metastatic involvement

Staging
- Imaging by ultrasound, CT, MRI, CXR

Blood
- LFT - common site of metastasis

Question 64

Q

Define molluscum contagiosum.

Answer

A

Caused by the molluscum contagiosum virus, a ubiquitous poxvirus that escapes immune destruction for months to years.

Answer 65

A

Lesions are cutaneous (less commonly mucosal).

Henderson-Patterson bodies - virally infected keratinocytes with central orifice (epidermal collections of molluscum bodies)

Caused via skin-to-skin or fomite contact in children, and by sexual transmission in adults.

Risk Factors:

Close contact with infected individual
Sexual contact with infected individual
HIV infection
Tropical climate
Swimming
Atopic dermatitis

Answer 66

A

1/3 patients develop symptoms of local erythema, swelling or pruritus.

Answer 67

A

Pearl-like, smooth papules
Umbilicated
Central dell
Surrounding erythema
Facial or groin distribution of lesions
Pruritus
Atopic dermatitis

Answer 68

A

Pearl-like, smooth papules
Umbilicated
Central dell
Surrounding erythema
Facial or groin distribution of lesions
Pruritus
Atopic dermatitis

Answer 69

A

Curettage biopsy
Tzanck stain
Haematoxylin and eosin staining
HIV test

Answer 70

A

Localised injury to the skin and / or underlying tissue usually over a body prominence, as a result of pressure or of pressure in combination with shear stress.

Most common over body prominence, but can develop on any part of the body, including mucosal surfaces.

Can be small, superficial wounds or blisters involving only epidermal elements or larger wounds, covered or filled with necrotic tissue and involving deeper tissues such as fascia, muscle or bone.

Answer 71

A

Stage 1 - non-blanchable redness of intact skin, typically over a bony prominence

Stage 2 - partial thickness loss of dermis presenting as a shallow, open ulcer with a red/pink wound bed, without slough, or an intact or open / ruptured sero-sanguinous blister

Stage 3 - full thickness skin loss with visible subcutaneous fat, bone/tendon/muscle not exposed

Stage 4 - full thickness tissue loss with exposed bone/tendon/muscle

Risk Factors:

Immbolity
Sensory impairment
Older age
Surgery
Intensive care stay
Malnourishment
History of previous pressur ulcers
Environmental factors - e.g. the nature of the surface on which the pateint has been sitting or lying
Faecal or urinary incontinence
Diabetes
Peripheral vascular disease

Answer 72

A

Use of non-pressure-relieving support surface
Localised skin changes on areas subjected to pressure
Shallow open wound or tissue loss on areas subjected to pressure
Full-thickness wound on areas with involvement of major tissues on areas subjected to pressure with or without undermining (tunnelling)
Localised tenderness and warmth around area of wound
Increased exudate and / or foul odour

Answer 73

A

Use of non-pressure-relieving support surface
Localised skin changes on areas subjected to pressure
Shallow open wound or tissue loss on areas subjected to pressure
Full-thickness wound on areas with involvement of major tissues on areas subjected to pressure with or without undermining (tunnelling)
Localised tenderness and warmth around area of wound
Increased exudate and / or foul odour

Answer 74

A

Clinical diagnosis
Wound swab
ESR - >100mm/hour in osteomyelitis
WBC - >15.0 x 10^9/L in osteomyelitis
Serum glucose - elevated in diabetes
Deep tissue biopsy
MRI

Answer 75

A

A chronic inflammatory skin disease, which has characteristic lesions and may be complicated by arthritis.

Answer 76

A

Unknown. Genetic, environmental factors and drugs (e.g. may be triggered by Streptococcal infections, antimalarial agents, B-blockers, lithium).

Excess proliferation of epidermal cells (rapid cell turnover possible mediated by cytokines released by lymphocytes in the dermis) and accelerated upward migration of immature keratinocytes.

Risk Factors:

Guttate psoriasis - Streptococci sore throat
Palmoplantar pustulosis - smoking, middle-aged women, autoimmune thyroid disease, SAPHO
Generalised pustular - hypoparathyroidism

SAPHO = synovitis, acne, palmoplantar pustulosis, hyperostosis, osteitis - chronic recurrent multifocal inflammation of bones (e.g. sternoclavicular, sacroiliac joint)

Answer 77

A

1-2% population

Peak age of onset = 20 years

Answer 78

A

Itching
Tender skin
Pinpoint bleeding with removing scales (Auspitz phenomenon)
Skin lesions may develop at the site of trauma / scars (Koebner phenomenon)

Answer 79

A

Discoid / Nummular Psoriasis:

Symmetrical
Well-demarcated
Erythematous plaques
Silvery scales over extsnor surface - knee, elbows, scalp, sacrum

Flexural Psoriasis:
- Less scaly plaques in axilla , groins, perianal, genital skin

Guttate:
- Small (<1cm) drop-like lesions over trunk, limbs

Palmoplantar:

Erythematous plaques
Pustules
Palms and soles

Generalized Pustular Psoriasis:
- Pustules distributed over limbs and torso

Nail:

Pitting
Oonycholysis - lifting off of the nail plate from the nail bed
Subungual hyperkeratosis
Salmon patch on the nail

Joints:

Seronegative arthritis with 6 possible presentations:
1) Monoarthritis
2) Distal asymmetrical oligoarthritis (distal interphalangeal joints)
3) Dactylitis (interphalangeal arthritis and flexor tenosynovitis)
4) Rheumatoid arthritis-like (symmetrical polyarthritis)
5) Arthritis mutilans (telescoping of the digits)
6) Anklyosing spondylitis

Poor correlation between joint and skin involvement.

Answer 80

A

Majority of patients do not need any investigations.

Guttate Psoriasis:

Anti-streptolysin-O titre
Throat swab

Flexural Lesions:
- Skin swabs - exclude candidiasis

Nail:
- Analyse nail clippings to exclude onychomycosis (fungal infection)

Joint Involvement:

Rhuematoid factor (negative)
Radiographs (distal interphalangeal joints)
Erosions
Perarticular osteoporosis
Pencil-in-cup deformity - whittling and cupping of the phalanges
Sacroilitis

Answer 81

A

Malignancy of the epidermal keratoinocytes of the skin.

Marjolin’s Ulcer - a squamous cell carcinoma that arises in an area of chronically inflammed or scarred skin.

Answer 82

A

Bowen’s Disease - intra-epidermal carcinoma in situ

Proliferation of atypical keratinocytes
Basement membrane intact
Solitary or multiple red-brown scaly patches

Squamous Cell Carcinoma

Malignant keratinocytes invade locally into the dermis
Spread to local lymph nodes
Distally metastasies - e.g. lungs, liver
Staging on TNM

Risk Factor:

UV radiation from sunlight exposure
Actinic keratoses - sun-induced precancerous lesions
Radiation
Carcinogens - e.g. tar derivatives, cigarette smoke, soot, industrial oils, arsenic
Chronic skin disease - e.g. lupus, peukoplakia
Human Papilloma Virus
Long-term immunosuppression - e.g. transplant recipients, HIV
DNA repair genetic defects - e.g. xeroderma pigmentosum

Answer 83

A

2nd most common cutaneous malignancy - 20% of skin cancer

Often occurring in middle-aged and elderly light-skinned individuals.

Incidence 1 in 4000 annually

M:F 2-3:1

Answer 84

A

Skin lesion
Ulcerated
Recurrent bleeding or non-healing

Answer 85

A

Variable appearance
Ulcerated
Hyperkeratotic
Crusted or scaly
Non-healing lesion
Often on sun-exposed areas
Palpate for local lymphadenoapthy

Answer 86

A

Variable appearance
Ulcerated
Hyperkeratotic
Crusted or scaly
Non-healing lesion
Often on sun-exposed areas
Palpate for local lymphadenopathy

Answer 87

A

A skin condition consisting of erythematous, blanching, oedematous, non-painful, pruritic lesions that develop rapidly, usually over minutes.

Typically lasts less than 24hours and leaves no residual skin markings upon resolutions.

Acute episodes - period of less than 6 weeks, caused by specific stimulus and are self-limiting.

Chronic episodes - period of over 6 weeks, not attributable to a specific stimulus.

Answer 88

A

Acute:

Lasts less than 6 weeks
Hypersensitivity reaction to a specific trigger
Viral infections

Chronic :

Daily or near-daily episodes of hives occuring for 6 weeks or more
Complex aetiology

Risk Factors:

Positive family history
Female sex
Exposure to drug or food trigger
Recent viral infection
Recent insect bite or sting

Answer 89

A

A recent studies reported that the lifetime prevalence of all types of urticaria was 8.8% to 10.8%, with a female predominance and a mean age of 35 to 39 years.

Angio-oedema - swelling involving the deeper layers of the subdermis and occurs in association with urticaria in 40% of cases. Involves face and neck, potentially compromise airway.

Answer 90

A

Pruritus - unpleasant sensation of the skin that provokes the urge to scratch
Resolution in 24 hours
Swelling of face, tongue or lips
Erythematous oedematous lesions
Blanching lesions
Stridor

Answer 91

A

Pruritus - unpleasant sensation of the skin that provokes the urge to scratch
Resolution in 24 hours
Swelling of face, tongue or lips
Erythematous oedematous lesions
Blanching lesions
Stridor

Answer 92

A

FBC - normal, eosinophilia, neutrophilia
ESR - elevated or normal
CRP - elevated or normal
C4 - decreased in hereditary and acquired angio-oedema
TSH - elevated or normal
ANA - anti-nuclear antibodies - positive in rheumatological disease
Skin prick testing - may be positive
Allergen avoidance diet
Serum tryptase
Skin biopsy
C1 esterase inhibitor level and function, C1q levels
Specific IgE to suspected allergen

Answer 93

A

Primary infection is called vaircella (chicken pox).

Reactivation of the dormant virus in the dorsal root ganglia, causes zoster (shingles).

Answer 94

A

Herpes ds-DNA virus
Highly contagious
Transmission by aerosol inhalation or direct contact with vesicular secretions

Viral inhalation and infection of the URT.
Replication in regional lymph nodes, liver and spleen.
Week 2-3 - spreads to skin, producing rash and then leading to clinical resolution.
Remains latent in dorsal root ganglia.
Reactivation causes virus to travel down sensory axon to produce dermatomal shingles rash.

Answer 95

A

Chickenpox peak incidence occurs at 4-10 years.
Shingles peak incidence at >50 years.
90% of adults are VZV IgG positive (previously infected).

Answer 96

A

Incubation period 14-21 says

Chicken Pox:

Prodromal malaise
Mild pyrexia
Sudden appearance of an intensely itchy spreading rash
Affecting the face and trunk more than the extremities, the oropharynx, conjunctivae, genitourinary tract
Vesicles weep and crust over, forming new vesicles
Contagious from 48h before the rash and until all the vesicles have crusted over - within 7-10 days

Shingles:

May occur after a period of stress
Tingling / hyperaesthesia in a dermatomal distribution
Painful skin lesions
Recovering in 10-14 days

Answer 97

A

Chicken Pox:

Macular papular rash
Evolves into crops of vesicles
Areas of weeping and crusting
Skin excoriation - from scratching
Mild pyrexia

Shingles:

Vesicular macular papular rash
Dermatomal distribution
Skin excoriation

Answer 98

A

Both chickenpox and shingles usually clinical diagnosis.

Vesicle Fluid

Electron microscopy
Direct immunofluorescence
Cell culture
Viral PCR - all rarely necessary

Chicken Pox

Consider HIV testing
Especially in adults with prior history of varicella infection

Answer 99

A

Chicken Pox:

Children - treat symptoms with calamine lotion, analgesia, antihistamines
Adults - consider aciclovir, valaciclovir, famciclovir if within 24h of rash onset especially if elderly, smoker, immunocompromised or pregnant

Shingles:

Aciclovir, valaciclovir, famciclovir if within 72h of rash onset if elderly, immunocompromised or ophthalmic involvement
Low-dose amitriptyline if in moderate / severe discomfort
Simple analgesia (paracetamol)

Prevention:

VZIG may be indicated in immunosuppressed and pregnant women exposed to varicella zoster
Chickenpox vaccine licensed in the UK, but no guidelines avaliable for appropriate use

Answer 100

A

Chicken Pox:

Secondary infection
Scarring
Pneumonia
Encephalitis
Cerebellar syndrome
Congenital varicella syndrome

Shingles:

Postherpetic neuralgia
Zoster opthalmicus - rash involves ophthalmic division of Trigeminal Nerve (CN V)
Ramsay Hunt’s Syndrome - reactivation in geniculate ganglion causing zoster of the ear and facial nerve palsy (vesicles behind pinna of ear or in canal)
Sacral zoster may lead to urinary retention
Motor zoster - muscle weakness of myotome at the similar level as involved dematome

Answer 101

A

Depends on complications.

Worse in pregnancy, elderly and immunocompromised.

Answer 102

A

Infection with candida, especially as causing oral or vaginal thrush.

Answer 103

A

Dimorphic fungus (yeast) colonizes approx. 30% individuals.

Colonization begins shortly after birth and persists throughout life
Found in respiratory, GI, genitourinary tracts and the skin and mucous membranes
Exists in both yeast (blastospore) phase and hyphal (mycelial) phase, depending on surrounding conditions
Immunocompetent individuals provide effective immune surveillance against Candida
Any immune defect can lead to infection and visible disease

Risk factors:

Antibiotics
Corticosteroids
Dental prostheses
Chemotherapy
Radiation treatment
HIV

Answer 104

A

Rise in Candida infections - due to diabetes, malignancy, chemotherapy, human immunodeficiency virus

200 species - most common C. albicans.

Answer 105

A

Areas of heat and humidity and maceration
Burning
Itching
Irritation
Redness and swelling
Pain and soreness
Rash

Answer 106

A

Cutaneous

Under breasts
In gluteal and inguinal folds
Diaper area
Under pannus
Armpit
Erythema with satellite papules
Overlying white plaques - intertrigo

Oral

Thrush
Infants and elderly

Answer 107

A

Superficial scraping
Add saline - see pseudohyphae and yeast under microscope
KOH added to nail or skin specimens to help dissolve the keratin and visualise the yeast
Calcolfluor white - rapid diagnosis with a fluorescent microscope
Culture and sensitivities
Skin biopsy with periodic acid-Schiff (PAS) staining

Brainscape's Knowledge GenomeTM

Dermatology Flashcards

Brainscape's Knowledge Genome^TM