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M. LAADHARI, A. AISSA, M. KHERIFECH, I. MEZHOUD, K. BEN HELAL*, M. ALLANI, R. ALOUINI. Medical . Imaging . Ibn. El . Jazzar. Hospital . Kairouan * Department – PowerPoint PPT presentation

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1
Venous vascular malformation type of soft tissue
discovery at puberty
  •  M. LAADHARI, A. AISSA, M. KHERIFECH, I. MEZHOUD,
    K. BEN HELAL, M. ALLANI, R. ALOUINI
  • Medical Imaging Ibn El Jazzar Hospital Kairouan
  • Department of Pediatrics Ibn El Jazzar Hospital
    Kairouan
  • Tunisia
  • PAN ARAB 2012- PEDIATRICS PD 9

2
INTRODUCTION
  • Vascular malformations are a spectrum of unknown
    injury interesting mainly the pediatric
    population
  • Venous malformations are the most common
    vascular malformations
  • In case of complex or atypical clinical
    presentation, the doppler ultrasound and MRI are
    the two noninvasive imaging techniques which are
    essential
  • To achieve the positive diagnosis towards
    differential diagnosis
  • To make an assessment of local and regional
    expansion referred to pre-therapeutic and
    prognostic and monitor spontaneous or on
    treatment of injuries

3
OBJECTIVES
  • Illustrate a case of vascular malformation
    hemodynamically inactive venous type.
  • Demonstrate the role of different imaging means
    (standard X-ray, doppler ultrasound,
    cross-sectional imaging) in the diagnostic
    confirmation.

4
OBSERVATION
  • A 12-year-old patient without a history disease,
    which was presented to the ED with a painful
    swelling of the forearm lasting for two days with
    a history of trauma two weeks ago.
  • Clinical examination swelling of the medial
    surface soft, movable relative to the two planes,
    painful without cutaneous signs in regard.
  • An X-ray standard, a doppler ultrasound, a CT
    scan supplemented by an MRI were performed.

5
  • OBSERVATION
  • X-ray standard face of the forearm
  • Soft tissue mass with round opacity tone calcium
    without adjacent bone changes.

6
  • OBSERVATION
  • Doppler Ultra sound
  • Multiple structures tubulated, tortuous
    hypoechoic, heterogeneous, infiltrating the
    subcutaneous fat, compressible with multiple
    hyperechoic spots followed by posterior acoustic
    shadowing (phlebolites).
  • No flow at color Doppler and pulse.

7
  • OBSERVATION
  • C T scann
  • Lesion on the soft tissu, containing many
    heterogeneous hyperdense calcifications of
    varying size, with enhancement after injection
    discreet locations.

8
  • OBSERVATION
  • M R I(1,5T)

Sequence -coronale -STIR-
Sequence -coronale -FSE T1-
  • Training oval in the subcutaneous and muscular
    tissue composed of contiguous structures
    serpiginous franc hyperT2, isoT1 with
    intralesional structures in focal hypoT2 EG and
    T2 are compatible with phleboliths.

9
  • OBSERVATION
  • M R I

T1
Sequence axiale-FSE T1,FSET2 and T2
T2
10
  • OBSERVATION
  • M R I

Axial-FSE T1 Fatsat after Gadolinium
MIP
Precoce and moderate enhancement, heterogeneous
and "clumps" after injection.
Coronal-FSE T1 Fatsat after Gadolinium
11
  • OBSERVATION
  • M R I

Coronal-FSE T1 Fatsat after Gadolinium
12
DISCUSSION
  • Prerequisite know the classification of
    superficial vascular abnormalities.
  • Many sources of terminological confusion
    misdiagnosis and inappropriate treatment.

13
Classification (1996) adopted by the
International Society for the Study of Vascular
Anomalies (ISSVA)
DISCUSSION
  • VASCULAR TUMORS abnormal endothelial cell
    proliferation
  • Vascular Malformations  embryological vessel
    abnormalities without abnormal cell proliferation

14
DISCUSSION Classification Vascular tumor
  • Infantile hemangioma the most common tumor in
    infants
  • Congenital hemangiomas (RICH and NICH),
    kaposiform hemangioendothelioma, tufted angioma
  • Exeptionnel hemangiopericytoma, fibrosarcoma,
    rhabdomyosarcoma infant

15
DISCUSSION Classification Vascular
malformations
  •  Classified according to hemodynamic data
  • (classification more relevant)
  • Slow flow malformations (hemodynamically
    inactive) capillary, venous ,lymphatic,
    combination of these malformations
  • Fast flow malformations (hemodynamically
    active)
  • Those with a blood component
  • Fistula or arteriovenous malformation

16
DISCUSSIONVASCULARMALFORMATIONS
17
DISCUSSION Vascular Malformation General
  • Congenital lesions
  • Present at birth
  • Always sometimes late clinical manifestation
    (until adolescence)
  • Lack of spontaneous regression, persistence
    throughout life with growth proportional to that
    of the child
  • Possible phases of thrust if trauma, infection,
    hormonal changes (puberty, pregnancy)

18
DISCUSSION Vascular Malformation General
  • Treatment usually necessary
  • Treatment is conditioned by hemodynamic
    characteristics of the vascular malformations
  • ? Importance of the distinction between
    congenital malformations and slow flow to fast
    flow

19
  • DISCUSSION
  • A slow flux malformation of capillary type
  • Place of imaging very limited
  • Superficial anomaly hardly visible on imaging
    (sometimes skin thickening and subcutaneous)
  • Search for underlying vascular malformation or
    associated anomalies (vascular syndromes)

20
  • DISCUSSION
  • A slow flux malformation of Venous type
  • Most common vascular malformation
  • Old "cavernous hemangioma" (confusing
    terminology)
  • Dysplastic veins venous ectasia or true venous
    lakes ( cavities with vascular endothelial
    lining)
  • Often evident at birth
  • Often asymptomatic, sometimes painful if
  • Thrust thrombosis secondary to intralesional or
    hormonal changes
  • Depth extension of the muscle
  • Joint damage
  • Headquarters head and neck region (40),
    extremities (40), trunk (20)

21
  • DISCUSSION
  • A slow flux malformation of Venous type
  • Two categories
  • Heredatery veinous malformations
  • Venous malformations common (our case)
  • The most common
  • Location Cervicofacial and members
  • Often later onset
  • Usual complications thrombosis in situ ? always
    find a localized intravascular coagulation
  • Treatment only in cases of functional impairment
    or significant aesthetic

22
  • DISCUSSION
  • A slow flux malformation of Venous type
  • Members
  • Clinical presentation
  • Possible with cutaneous, subcutaneous, muscle
    and joint
  • Pain due to thrombosis localized to gravity or
    nerve compression
  • In case of joint damage recurrent effusions and
    hemorrhagic reaction with possible cartilage
    destruction (type hemophilic arthropathy)

23
  • DISCUSSION
  • A slow flux malformation of Venous type
  • X-ray standard
  • Mass of soft tissue
  • Non-specific but inconstant pathognomonic
    phleboliths (round opacities tone calcium)
  • Possible bone remodeling adjacent lesions
    extended

24
  • DISCUSSION
  • A slow flux malformation of Venous type
  • Color and pulsed doppler ultrasound
  • Two types of venous malformations
  • Cavitary
  • Gaps
  • Phlebolite
  • Slow venous flow monophasic
  • No flow (16) thrombosis or technical
    limitations (very slow flow below the detection
    flux) gt to Valsalva maneuver
  • Component two-phase flow capillary-associated
    (slow arterial flow)
  • Dysplasique
  • Multiple varicose dilatations
  • Multiple structures tubulées tortuous, anechoic,
    infiltrating the subcutaneous fat, muscle-tendon
    structures ...
  • Slow venous flow

25
  • DISCUSSION
  • A slow flux malformation of Venous type
  • CT scann
  • Little use
  • More sensitive than plain radiography for
    detecting phleboliths
  • Detection of any fatty component and detection
    of bone underlying

26
  • DISCUSSION
  • A slow flux malformation of Venous type
  • IRM
  • PRECONISED PROTOCOLE
  • Importance of T2 FS or STIR sequences
  • SE T1 staging (anatomical balance), EG T2
    (phleboliths, hemosiderin)
  • T1 FS gado (evaluation of perfusion)
  • 3D dynamic MR angiography with injection
  • EG 3D T1 gadolinium bolus (2 ml / s) and
    subtraction
  • Dynamic MRI evaluation of time between the
    onset of arterial enhancement and early
    enhancement of the lesion
  • Early if ltor 6 s component malformation with
    arterial or capillary
  • Late ifgt 6 s pure venous malformation

27
  • DISCUSSION
  • A slow flux malformation of Venous type
  • IRM
  • HABITUEL ASPECTS
  • Serpiginous structures, tubulated or
    multilocular masses in connection with venous
    lakes separated by septa
  • Isosignal or hypo-signal on T1, frank
    hyper-signal on T2.
  • More heterogeneous signal on T1 if bleeding or
    thrombosis.
  • Hypo-signal areas on T2 (phleboliths, thrombi,
    septa).
  • Hypointense on all sequences (phleboliths).
  • EG asignal on T2 (slow flow).
  • Progressive enhancement "patchy" or "clumps" of
    circulating areas.

28
  • DISCUSSION
  • A slow flux malformation of Venous type
  • Per-cutanous phlebography
  • Not useful for diagnosis
  • Stage 1 of treatment by sclerotherapy (in
    puncture of the malformation with needle 20-22 G)
  • Optimal evaluation of the anatomy of the MV and
    its venous drainage

29
CONCLUSION
  • The superficial vascular abnormalities are a
    diagnostic and therapeutic challenge that must be
    based on a multidisciplinary approach.
  • Their diagnosis is based primarily on clinical
    examination.
  • Vascular malformations are usually present at
    birth and do not regress spontaneously.

30
CONCLUSION
  • Venous malformations are the most common
    vascular malformations and arteriovenous
    malformations are vascular malformations, the
    most dangerous, with unpredictable and difficult
    to treat.
  • It is important to distinguish between slow flow
    vascular malformations (capillary, venous,
    lymphatic) and vascular malformations fast flow
    (arteriovenous) that fall under different
    therapeutic management
  • ? Interest of 3D MR angiography with dynamic
    gadolinium-enhanced and high temporal resolution
    (5 s).
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