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PAPULOSQUAMOUS DISORDERS

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Title: PAPULOSQUAMOUS DISORDERS


1
PAPULOSQUAMOUS DISORDERS
  • DR.V.SUJA
  • PROFESSOR
  • DERMATOLOGY VENEREOLOGY

2
PAPULES, PLAQUES SCALING
  • EPIDERMOPOIESIS

3
PAPULOSQUAMOUS DISORDERS
  • Psoriasis
  • Lichen planus
  • Lichen nitidus
  • Lichen striatus
  • Expoliative dermatitis
  • Pityrasis rosea
  • Seborrhec dermatitis
  • DOS
  • Secondary syphilis
  • Durg reactions
  • Fungal infections

4
PSORIASIS
  • 3 PREVALENCE
  • VARIED PRESENTATION
  • VARIED TREATMENT MODALITIES
  • TREATMENT SHOULD BE INDIVIDUALISED
  • PATIENT EDUCATION IMPORTANT

5
DEFINITION
  • Chronic disorder
  • Affects skin joints
  • Multifactorial etiology
  • Unpredictable course
  • Remissions exacerbations
  • Most prevalent t cell mediated
  • Inflammatory disorder of skin

6
AETIOPATHOGENISIS
  • Exact cause-unknown
  • Genetic predisposition
  • Precipitating factors

7
AETIOPATHOGENISIS
  • Epidermal Factors
  • Transit Time lt13 Days To 2 Days
  • SCAg Leaks Bind To SCAbgtAg/Ab Complexes Bind
    To Complementgt PMNL Infiltration To Epidermisgt
    Epidermopoiesis
  • Dermal Factors

8
AETIOPATHOGENISIS
  • Dermal factors
  • capillary changes
  • arterial capillaries to venous capillaries
  • Leakage of PMNL to epidermisgtrapid epidermopoiesis

9
GENTIC FACTORS
  • Especially in arthropathic type
  • Multilocus model of inheritance
  • HLA-cw6 locus
  • Genetic code is critical in the devt of disease
  • Susceptible individuals in latent
    phenotype-prepsoriasis
  • Transmission to children varies

10
AETIOPATHOGENISIS
  • TRIGGER FACTORS
  • INFECTION
  • TRAJUMA
  • DRUGS
  • BETA BLOCKERS
  • ANTMALARIALS
  • LTHUM
  • NSAIDS
  • INTERLENION ON
  • PREGNACNY
  • HIV
  • SEASONAL

11
AETIOPATHOGENISIS
  • There is an aberration through the skin of
    patients with psoriasis that is modified to
    disease expression by circulating factors

12
AETIOPATHOGENISIS
  • ACTIVATED T CELLS ENTER SKIN
  • RELEASE CYTOKINES CHEMOKINGE
  • LEADS TO INFLAMMATION
  • COB CD4 CELLS MEDIATE EPIDERMAL HYPERPLASIA

13
AETIOPATHOGENISIS
  • EPIDERMAL KERATINOCYTES DERIVED CYTOKINGES
  • T CELL ACTIVATION
  • T CELL ACTIVATION (ANTIGEN PROCESSED BY
    LANGERHANS CELLS). CYTOKINES
  • ACTIVATE EPIDERMAL KERTINOCYTIES
  • CDS(KILLER) TLYM-AUTOREACTIVE WITH EPIDERMAL
    KERATINOCYTIES
  • EPIDERMAL ACTIVATION

14
AETIOPATHOGENISIS
  • ACTIVATEDSKIN HOMING PATHOGENIC T CELL
    POPULATION
  • LIBERATES CYTOKINES AND CHEMOKINES LEADS TO
  • INFLAMMATORY INFLTRATE EPSISRMAL
    PROLIERATION WIH ABNORMAL KERATNOCYTE
    DIFFERENTIAATION

15
CLINICAL LFEATURES
  • Psora-to itch
  • Extensor predilection
  • Varied presentation
  • Nail lesions common
  • Oral lesions rare
  • Joint
  • Pustular lesions
  • Exploitive dermatitis
  • Koebner phenomenon
  • Auspitiz sign

16
TYPES OF PSORIASIS
  • PS VULGARIS
  • FLXEURAL PS OR INVERSE PS
  • GUTTATE PS
  • SEBO PS
  • FOLLICULAR PS
  • EXFOLIATIVE PS
  • NAIL LPS
  • PALMOPLANTAR PS

17
NAIL CHANGES
  • PITTING
  • SUBUNGUAL HYPER KERATOSIS
  • ONYCHOLYSIS
  • YELLOWISH DISCOLORATION
  • OIL DROP SIGN

18
PS ARTHROPATHY-TYPES
  • DISTAL INTERPHALANGEAL
  • MONO/OLIGOARTICULAR
  • POLYARTICULAR
  • SACROILIATIS
  • RHEUMATOID ARTHRITIS TYPE
  • MUTLANS

19
COMPLICATIONS
  • PSYCHOLOGICAL STRESS
  • ARTHROPATHY
  • EXRFOLIATIVE DERMATITIS
  • PUSTULAR PS
  • LOCALISED
  • GENERALISED-VON-ZUMBUSCH
  • TYPE-EMERGENCY

20
TREATMENT
21
CHRONIC OR STABLE PS
  • TOPICL LKERATOLYTIC ANITIMITIOTICS
  • SYSTEMIC DRUGS AS TETRACYCLINES,OMEGA
    TRGLYDERIDES dapsone clofazimine
  • PHOTOTHERAPY
  • SYSTEMIC IMMUNOSUPPRESSANTS
  • METHOTREXATE,CYCLOSPORIN
  • RETINOIDS
  • PEPUVA
  • OTHER DRUGS AS HYDROXY UREA
  • BILOGICALS

22
TOPICAL AGENTS
  • TAR
  • CRUDE COAL TAR IN PETROLATUM
  • IN STABLE PS
  • MECHANISM
  • PHOTODYNAMIC
  • ANTIMITOTIC

23
APPLICATIONS OF TAR
  • SCALP-ALCOHOLIC EXTRACTS /TAR SHAMPOSS
  • USE VEGETABLE OL ON SCALP 1 hr PRIOR TO
    APPLICATION OF TAR
  • PALMOPLANTAR-TAR BATH OR OINTMENT (CURDE COAL TAR
    TO SOFT PARAFFIN 6-12) SALYCYLIC ACID
  • SALYCILIC ACID-3 gm
  • CRUDE COAL TAR -6 gm
  • VASELINE LUPTO-100gm

24
TAR
  • TAR BATH-LIQUOR LPICIS CARE 6-12 ml TO AGLAS OF
    WATER HALF LAN HOUR BATH AND EXPOSE TO SUN LIGHT
    FOR 20 MIN DAILY
  • AVOID TAR IN FACE INTERIGINOUS AREAS
  • GOKERMAN THERAPY
  • APPLY CRUDE COAL TAR FOLLOED BY UVB
  • HOSPITALISE
  • PRIOR TESTING IS NEEDED-3 OINT AS LOPEN PATCH
    TEST IN ABD WALL -24 hrs

25
TAR
  • COMPLICATIONS
  • PRIMARY IRRITATION
  • FOLLICULITIS
  • TAR ACNE
  • REVERSIBLE PIGMENTATION
  • EXDACERBATION OF LEWSIONS
  • BURNING
  • CARCINOGENICITY

26
TAR-CI
  • ERYTHRODERMA
  • PUSTULAR PS
  • UNSTABLE PS
  • FLEXURAL, SCROTAL FACE LESIONS
  • IRRITATION-GIVE TOPICAL STEROIDS

27
DITHRANOL
  • CIGNOLIN OR ANTHRALINE
  • CHRYAORABIN FROM ARAROBA TREE (TAWNY COLORED)-GOA
    POWDER
  • HIGHLY UNSTABLE-HYDROXY FREE RADICALS PRODUCED
    (ACT ON THE STEM CELL POPULLATION OF EPIDERMIS)
    THERAPEUTIC EFFECT/ STAINING
  • YELLOW LTO PURPLE BROWN STAINING
  • USE WITH CAUTION- BURNING

28
DITHRANOL
  • START WITH LOW CONC JUST FEELING OF WARMTH
  • ltCONTACT TIME OR COC
  • DONT APPLY TO NORMAL SKIN
  • FLEXURAL ARES-0.1-0.25 CREAM
  • CI IN MOIST AND INFLAMMED LESIONS

29
DITHRANOL
  • INGRAM REGIME
  • COAL LTAR BATH DRY
  • UVB
  • APPLY DITHRANCL LO.42 IN LASSERS PASTE TO
    STIFFEN
  • COVER WITH POWDER, STOCIKINET DRESSING
  • AFTER 24 HRS REMOVE IT VEG RPT
  • SHORT CONTACT THERAPY
  • 0-1-0.OR 2 CONC FOR SHOR PERIOD OF CONTACH
  • COMBINATOIN THERAPY
  • DITHRANOL CALCIPOTROIN/STEROIDS/STEROIDS/TAZAAROT
    ENE

30
TOPICAL RETINOIDS
  • SYNTHETIC / NATURAL COMPOUNDS WITH VITA ACTIVITY
  • TOPICAL RETINOIDS IN MINOR TYPE OF LPS
  • SYSTEMIC RETINOIDS IN SEVRE PS
  • 1990- TAZAROTENE
  • MODULATE EXPRESSION OF GENS THAT REGULATE CELL
    PROLIFERATION DIFFERENTIATION
  • SYSTEMIC ABS MINIMAL
  • CARCINOGENIC EFFECT RARE

31
TOPICAL RETINOIDS
  • INDICATIONS
  • CHRONIC STABLE PLAUE TYPEON TRUNK OR LIMBS UP TO
    20 OF BODY AREA
  • CL-PREGNANCY ECZEMATOUS LESIONS, ALLERGY SUNBURNS
  • MONOTHERAPY -0.5,0.1
  • COMBINATION THERAPY
  • ALTERNATIVE LWITH TOPICAL LSTEROIDS
  • UBV/UNA

32
VIT D3 ANALOGUES
  • VIT HORMONE
  • 1.25 (OH )2 D3 INHIBITS KERATIONOCYTE
    PROLIFERATION HELPS IN DIFFERENTIATION
  • CALCIPOTROIL-SYNTHETIC ANALOGUE OF
  • CALCITRIOL LESS ACTION IN CA METABOLISM
  • 550MI CROMGM/GIN AN OINTMENT IS SUFFIVCIENT
  • CAN BE USED IN FLEXURAL SITES ALSO ORIETMENT
    CREAM SOLUTION
  • AVODN IN PREGINANCY

33
SALICYLIC ACID
  • KERATOLYTIC ltCORNECYUITE ADHESION
  • WINTER GREENLEAVES
  • THICK HEPERKERATOTIC LESIONS
  • INSCALP,PALM SOLE
  • CAN BE COMBINED WITH STEROIDS , TAR
  • OTHER TOPICAL AGENTS
  • METHOTREXATE 0.25
  • ALLANTION

34
PHOTO/PHOTOCHEMOTHERAPY
  • PUVA ORAL LPSORALENUVA- PUVASOL
  • EYE CHECKYR CATARACT, MALIGNANCIES
  • 8-MOP 0.6 MG/KG 2 HRS PRIOR
  • 5 MOP1.2MG/KG 1 HR PRIOR
  • 11AM FOR 12 MIN
  • THRICE A WEEK
  • RESPONSED BY 20 TREATMENTS
  • TWICE A WEEK FOR 1 MON ONCE WEEKLY FOR ONE MON
  • CONTINUE FOR 2 MORE MONTHS
  • THEN TREATMENT FREE PERIOD OF 3 MON
  • BATH PVA-20 MIN IN 0.5 MG/L WATER SOLUTION OF 8-
    MOP DRY SKIN X EXPOSE TO UVA
  • CREAM PUVA

35
NARROW BAND UVB (31 NM) THERAPY
  • PHOTOTHERAPY OF CHOICE
  • REMISSIONOF SKIN LESIONS
  • LARGER PERIOD LOF REMISSION
  • CAN BE USED IN PREGENANCY CHILDREN, NO POST
    TRETMENT EYE
  • PROTECTION NEEDED
  • START WITH 0.7 MED
  • LATER gt BY 20-40 OF THE DOSE

36
METHOTREXATE
  • ERYTRODERMA PUSTULAR PS, ARTHROPATHY gt40 BOBY
    AREA INVT, FAILURE LOF OTHER MODES
  • DOSEAGE-
  • 12 HR APRT WEELY DOSE OF 7.5 TO 22.5 MG
  • SINGLE WEEKLY ORAL 25-37.5MG
  • WEEKLY PARENTERAL IM/IV 15-50MG

37
METHOTREXATE
  • CI-PREGNANCY RENAL D/S RECENT HEPATITIS LIVER
    CIRRHOSIS FIBROSIS, ALCOHOLISM PEPTIC ULCER,
    SEVERE INFECTIONS SEVERE ANEMIA LEUCOPENIA,
    THROMBOCYTOPENIA, UNWILLING TO ADOPT
    CONTRACEPTION
  • CUMULATIVE DOSE 1.5 GM LIVER BIOPSY

38
SYSTEMIC RETINOIDS
  • PROLIFERATION NORMALISES DIFFERENTIATION,
    IMMUNOMODULATION
  • ACT THROUGH CYTOPLASMIC NULEAR RETINOID
    RECEPTORS REGULATING GENE EXPRESSION
  • ETRETINATE
  • ACITRETIN-METABOLITE OF ETRETINATE

39
ACITRETIN ETRETINATE
  • STANDARD TREATMENT FOR MODERATE TO SEVERE PS
  • CHRONOC PLAQUES PS -COM,BINATION OF A/E WITH
    DIRANOL OR VIT D3 ANALOUES/TAR
  • ERYTHRODERMIC/SVERE PUSTULAR PS MONOTHERAPY
  • ALSO FOR MAINTENANCE THERAPY

40
ACITRETIN ETRETINATE
  • SIDE EFFECTS
  • CHELITIS DRYNESSOF MUCOSA EPISTAXIS, THIRST
    XEROSIS, PRURITUS, HAIR LOSS-ALL REVERSIBLE
    ONSTOPPING THERAPY
  • gtTRIGLYCERIDES, SOLOW FAT, LOW CHO DIET
  • DISH
  • CONTRACEPTION MUST BE BEGUN 1 MON BEFORE STRATING
    AND SHOULD BE CONTINUED FOR AT LEAST 2 YRS AFTER
    STOPPAGE IN WOMEN

41
ACITRETIN ETRETINATE
  • CI-SEVERE LIVER /RENAL D/S
  • DIABETES MELLITUS., HYPERILIPIDEMIAS
  • REGENANCY LACTATIONOR PLANNIN GOF PREG WITHIN 2
    YRS OF STOPPING THE DURG
  • DOSE ACITRETIN -0.25.0.6 MG/KG/DAY
  • ONCE CLEAREANCE-LOWER DOSE TO 0.2-0.4 MG/KG/DAY
    FOR 3-6 MON
  • CAN BE USED IN IMMUNOCOMPROMISED ALSO

42
ACITRETIN ETRETINATE
  • DRUG INTERACTIONS
  • TETRACYCLINES, PHENYTION, BARBITURATES, NSAIDS,
    KETOCONAZOL
  • E AND CYCLOSPORIN
  • SYSTEMIC CORTICOSTEROIDS
  • NO ROLE IN CHRONIC PLAQUE PS
  • SEVER PUSTULAR PS- ESPE IN PREG
  • ERYTHRODERMA WITH SVERE
  • SYSTEMIC COM

43
BALNEOTHERAPY BALNEOPHOTOTHERAPY
  • SALT WATER BATHgt EXPOSE TO SUNLIGHT
  • gt20 SALT WATER WATER BATHgtUVB
  • SEA WATER BATH NATURAL UUV EXPOSURE CLIMATO
    THERAPY
  • DEAD SEA TREATMET IN ISRAEL LASERS
  • STUBBORN PS PLAQUES NOT RESPONOING -308 NM
    EXCIMER LASERS

44
NAIL PS
  • TOPICAL LDIPS IN COAL TAR
  • IONTOPHERISIS OF MIX
  • TOPICAL CORTICOSTEROIDS UNDER OCCLUSION
  • TOPICAL 1 5 FUL/l TRIAMCINOLONE
  • PUVA
  • TAZAROTENE TOPICAL

45
IMMUNE ALTERING BIOLOGICAL THERAPY
  • PROTEINS THAT BIND TO EXTRACELLULAR TARGETS,
    BLOCK MOLECULAR ACTIVATION
  • CLASS 1 MONOCLONAL ANTIBODIES
  • CLASS 2 ANTIBODY LIKE FUSION
  • PROTEINS FUSED SEGMENTS OF
  • MOUSE AND HUMAN Ab
  • ALEF ACEPT ETANERCEPT

46
ALEFACEPT, ETANERCEPT
  • ALEFACEPT BLOCK MHC MOLECULE
  • COMPETIVE INHIBITOR OF INF-A
  • APPROVED BY USFDA
  • DOSE -25 MG TWICE WEEKLY BY S/C INJ FOR 12 WEEKS
  • COMPLICATIONS AS MULITIPLE SCLEROSIS , SKING CA,
    LUPUS, ARE SEVR

47
BIOLOGICALS
  • BIOLOGICALS LAREA A DISTANT HORIZON IN TE OF PS
  • EXFOLIVATIVE DERMATITIS
  • DERMATOLOGIC CAUSES
  • SYATEMIC DISEASE
  • IDIOPATHIC
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