Vascular malformation: Difference between revisions

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{{Vascular malformation}}
{{Vascular malformation}}
{{CMG}}; {{AE}} {{HMHJ}}, {{Anmol}}
{{CMG}}; {{AE}} {{HMHJ}}, {{Anmol}}


==Overview==
==Overview==
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{{Family tree | | | | | | | | | | | | | A01 | | | | | | | | | | | | | | |A01= Vascular malformations}}
{{Family tree | | | | | | | A01 | | | | | | | |A01= '''[[Vascular malformations]]'''}}
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{{Family tree | | | B01 | | | | B02 | | | | | B03 | | | | B04 | | | | | |B01=Simple vascular malformations|B02=Combined vascular malformations*|B03=Vascular malformations of major named vessels|B04=Vascular malformations asscoiated with other anomalies}}
{{Family tree | B01 | | B02 | | B03 | | B04 | |B01='''''[[Simple vascular malformations]]'''''|B02='''''[[Combined vascular malformations]]'''''|B03='''''Vascular malformations of major named vessels'''''|B04='''''[[Vascular malformations asscoiated with other anomalies]]'''''}}
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{{Family tree | |!| | | I02 | | I03 | | I04 | |I02=<table class="wikitable">
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<tr><td>'''CM + VM'''</td><td>Capillary-venous malformation</td><td>CVM</td></tr>
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<tr><td>'''CM + LM'''</td><td>Capillary-lymphatic malformation</td><td>CLM</td></tr>
{{Family tree | | | C01 | | | C02 | | | C03 | | | C04 | | | C05 | | | | |C01=Capillary malformations (CM)|C02=Lymphatic malformations (LM)|C03=Venous malformations (VM)|C04=Arteriovenous malformations (AVM)|C05=Arteriovenous fistula}}
<tr><td>'''CM + AVM'''</td><td>Capillary-arteriovenous malformation</td><td>CAVM</td></tr>
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<tr><td>'''LM + VM'''</td><td>Lymphatic-venous malformation</td><td>LVM</td></tr>
{{Family tree | | |)| D01 | |)| E01 | |)| F01 | |)| G01 | |)| H01 | | | |D01=Nevus simplex / salmon patch, “angel kiss”, “stork bite”|E01=<table>
<tr><td>'''CM + LM + VM'''</td><td>Capillary-lymphatic-venous malformation</td><td>CLVM</td></tr>
<tr><td>Common (cystic) LM </td></tr>
<tr><td>'''CM + LM + AVM'''</td><td>Capillary-lymphatic-arteriovenous malformation</td><td>CLVM</td></tr>
<tr><td>• Macrocystic  LM<td></tr>
<tr><td>'''CM + VM + AVM'''</td><td>Capillary-venous-arteriovenous malformation</td><td>CVAVM</td></tr>
<tr><td>• Microcystic LM<td></tr>
<tr><td>'''CM + LM + VM + AVM'''</td><td>Capillary-lymphatic-venous-arteriovenous malformation</td><td>CLVAVM</td></tr>
<tr><td>• Mixed cystic LM<td></tr>
</table>|I03=<br>(also known as "channel type" or "truncal" vascular malformations)<br><table>
</table>|F01=Common VM|G01=Sporadic|H01=Sporadic}}
<tr><td>'''Affect'''</td></tr>
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<tr><td>• Lymphatics<td></tr>
{{Family tree | | |)| D02 | |)| E02 | |)| F02 | |)| G02 | |)| H02 | | | | |D02=<table>
<tr><td>• Veins</tr>
<tr><td>Cutaneous and/or mucosal CM (also known as “port-wine” stain) </td></tr>
<tr><td>• Arteries</tr>
<tr><td>• Nonsyndromic CM<td></tr>
<tr><td>'''Anomalies of'''</td></tr>
<tr><td>• CM with CNS and/or ocular anomalies (Sturge-Weber syndrome)<td></tr>
<tr><td>• Origin<td></tr>
<tr><td>• Course<td></tr>
<tr><td>• Number<td></tr>
<tr><td>• Diameter (aplasia,<br>hypoplasia, stenosis,<br>ectasia / aneurysm)<td></tr>
<tr><td>• Valves<td></tr>
<tr><td>• Communication (AVF)<td></tr>
<tr><td>• Persistence (of<br>embryonal vessel)<td></tr>
</table>|I04=<table class="wikitable">
<tr><td>'''[[Klippel-Trenaunay syndrome]]'''</td><td>CM + VM +/-LM + limb overgrowth</td></tr>
<tr><td>'''[[Parke's Weber syndrome]]'''</td><td>CM + AVF + limb overgrowth</td></tr>
<tr><td>'''[[Servelle-Martorell syndrome]]'''</td><td>Limb VM + bone undergrowth</td></tr>
<tr><td>'''[[Sturge-Weber syndrome]]'''</td><td>Facial + leptomeningeal CM + eye anomalies +/-bone and/or soft tissue overgrowth</td></tr>
<tr><td>'''[[Maffucci syndrome]]'''</td><td>VM +/-spindle-cell hemangioma + enchondroma</td></tr>
<tr><td>'''[[CLOVES syndrome]]'''</td><td>LM + VM + CM +/-AVM+ lipomatous overgrowth</td></tr>
<tr><td>'''[[Proteus syndrome]]'''</td><td>CM, VM and/or LM + asymmetrical somatic overgrowth</td></tr>
<tr><td>'''[[Bannayan-Riley-Ruvalcaba syndrome]]'''</td><td>lower lip CM + face and neck LM + asymmetry and partial/generalized overgrowth</td></tr>
<tr><td colspan="2">'''Limb CM + congenital non-progressive limb overgrowth'''</td></tr>
<tr><td colspan="2">'''Macrocephaly-CM (M-CM / MCAP)'''</td></tr>
<tr><td colspan="2">'''Microcephaly-CM (MICCAP)'''</td></tr>
</table>|}}
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{{Family tree | | C01 | | C02 | | C03 | | C04 | | C05 | |C01=[[Capillary malformations]] (CM)|C02=[[Lymphatic malformations]] (LM)|C03=[[Venous malformations]] (VM)|C04=[[Arteriovenous malformation]] (AVM)|C05=[[Arteriovenous fistula]]}}
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{{Family tree | |)| D01 |)| E01 |)| F01 |)| G01 |)| H01 |D01=[[Nevus simplex]] / [[salmon patch]], “[[angel kiss]]”, “[[stork bite]]”|E01=<table>
<tr><td>[[Common (cystic) LM]] </td></tr>
<tr><td>• [[Macrocystic  LM]]<td></tr>
<tr><td>• [[Microcystic LM]]<td></tr>
<tr><td>• [[Mixed cystic LM]]<td></tr>
</table>|F01=[[Common VM]]|G01=Sporadic|H01=Sporadic}}
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{{Family tree | |)| D02 |)| E02 |)| F02 |)| G02 |)| H02 |D02=<table>
<tr><td>[[Cutaneous and/or mucosal CM]] (also known as [[“port-wine” stain]]) </td></tr>
<tr><td>• [[Nonsyndromic CM]]<td></tr>
<tr><td>• CM with CNS and/or ocular anomalies ([[Sturge-Weber syndrome]])<td></tr>
<tr><td>• CM with bone and/or soft tissues overgrowth <td></tr>
<tr><td>• CM with bone and/or soft tissues overgrowth <td></tr>
<tr><td>• Diffuse CM with overgrowth (DCMO) <td></tr>
<tr><td>• [[Diffuse CM with overgrowth]] ([[DCMO]]) <td></tr>
</table>|E02=Generalized lymphatic anomaly (GLA)<br>Kaposiform lymphangiomatosis (KLA)|F02=Familial VM cutaneo-mucosal (VMCM)|G02=In HHT|H02=In HHT|}}
</table>|E02=[[Generalized lymphatic anomaly]] ([[GLA]])<br>[[Kaposiform lymphangiomatosis]] ([[KLA]])|F02=[[Familial VM cutaneo-mucosal]] ([[VMCM]])|G02=In [[HHT]]|H02=In [[HHT]]|}}
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{{Family tree | | |)| D03 | |)| E03 | |)| F03 | |)| G03 | |)| H03 | | | | | |D03=<table>
{{Family tree | |)| D03 |)| E03 |)| F03 |)| G03 |)| H03 |D03=<table>
<tr><td>Reticulate CM </td></tr>
<tr><td>[[Reticulate CM]] </td></tr>
<tr><td>• CM of MIC-CAP (microcephaly-capillary malformation)<td></tr>
<tr><td>• CM of MIC-CAP (microcephaly-capillary malformation)<td></tr>
<tr><td>• CM of MCAP (megalencephaly-capillary malformation-polymicrogyria)<td></tr>
<tr><td>• CM of MCAP (megalencephaly-capillary malformation-polymicrogyria)<td></tr>
</table>|E03=LM in Gorham-Stout disease|F03=Blue rubber bleb nevus (Bean) syndrome VM|G03=In CM-AVM|H03=In CM-AVM|}}
</table>
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|E03=LM in [[Gorham-Stout disease]]|F03=[[Blue rubber bleb nevus (Bean) syndrome]] VM|G03=In [[CM-AVM]]|H03=In [[CM-AVM]]|}}
{{Family tree | | |)| D04 | |)| E04 | |)| F04 | |`| G04 | |`| H04 | | | | | | |D04=CM of CM-AVM|E04=Channel type LM|F04=Glomuvenous malformation (GVM)|G04=Others|H04=Others|}}
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{{Family tree | |)| D04 |)| E04 |)| F04 |`| G04 |`| H04 |D04=[[CM of CM-AVM]]|E04=Channel type LM|F04=[[Glomuvenous malformation]] ([[GVM]])|G04=Others|H04=Others|}}
{{Family tree | | |)| D05 | |)| E05 | |)| F05 | | | | | | | | | | | | | | | | |D05=Cutis marmorata telangiectatica congenita (CMTC)|E05=“Acquired” progressive lymphatic anomaly (so called acquired progressive "lymphangioma")|F05=Cerebral cavernous malformation (CCM) |}}
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{{Family tree | |)| D05 |)| E05 |)| F05 | | | | | | | | |D05=[[Cutis marmorata telangiectatica congenita]] ([[CMTC]])|E05=[[“Acquired” progressive lymphatic anomaly]] (so called [[acquired progressive "lymphangioma"]])|F05=[[Cerebral cavernous malformation]] ([[CCM]]) |}}
{{Family tree | | |)| D06 | |)| E06 | |)| F06 | | | | | | | | | | | | | | | | |D06=Others|E06=Primary lymphedema |F06=Familial intraosseous vascular malformation (VMOS)|}}
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{{Family tree | |)| D06 |)| E06 |)| F06 | | | | | | | | |D06=Others|E06=[[Primary lymphedema]] |F06=[[Familial intraosseous vascular malformation]] ([[VMOS]])|}}
{{Family tree | | |`| D07 | |`| E07 | |)| F07 | | | | | | | | | | | | | | | | |D07=<table>
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<tr><td>Telangiectasia </td></tr>
{{Family tree | |`| D07 |`| E07 |)| F07 | | | | | | | | |D07=<table>
<tr><td>• Hereditary hemorrhagic telangiectasia (HHT) <td></tr>
<tr><td>[[Telangiectasia]] </td></tr>
<tr><td>• [[Hereditary hemorrhagic telangiectasia]] (HHT) <td></tr>
<tr><td>• Others<td></tr>
<tr><td>• Others<td></tr>
</table>|E07=Others|F07=Verrucous venous malformation (formerly verrucous hemangioma)|}}
</table>|E07=Others|F07=[[Verrucous venous malformation]] (formerly [[verrucous hemangioma]])|}}
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{{Family tree | | | | | | | | | | | | |`| F08 | | | | | | | | | | | | | | | | |F08=Others|}}
{{Family tree | | | | | | | | | |`| F08 | | | | | | | | |F08=Others|}}
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'''Abbreviations:''' CM:capillary malformation; VM:venous malformation; CVM:capillary venous malformation; LM:lymphatic malformation; CLM:capillary lymphatic malformation; AVM:arteriovenous malformation; CAVM:capillary arteriovenous malformation; LVM:lymphatic venous malformation; CLVM:capillary lymphatic venous malformation; CVAVM:capillary venous arteriovenous malformation; CLVAVM:capillary lymphatic venous arteriovenous malformation; AVF:arteriovenous fistula; CLOVES:congenital lipomatous overgrowth, vascular malformations, epidermal nevi, skeletal/scoliosis and spinal abnormalities; M-CM:macrocephaly-capillary malformation; MCAP:megalencephaly-capillary malformation-polymicrogyria; MICCAP:microcephaly-capillary malformation; CNS:central nervous system; DCMO:diffuse capillary malformation with overgrowth; CM-AVM:capillary malformation-arteriovenous malformation; CMTC:cutis marmorata telangiectatica congenita; HHT:hereditary hemorrhagic telangiectasia; GLA:generalized lymphatic anomaly; KLA:kaposiform lymphangiomatosis; VMCM:venous malformation cutaneo mucosal; GVM:glomuvenous malformation; CCM:cerebral cavernous malformation.
'''Adapted from International Society for the Study of Vascular Anomalies'''<ref name="urlClassification | International Society for the Study of Vascular Anomalies">{{cite web |url=http://www.issva.org/classification |title=Classification &#124; International Society for the Study of Vascular Anomalies |format= |work= |accessdate=}}</ref>


=Simple Vascular Malformations=
=Simple Vascular Malformations=
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=Combined Vascular Malformations=
=Combined Vascular Malformations=
{| class="wikitable"
{| class="wikitable"
! colspan="3" style="background:#4479BA; color: #FFFFFF;" align="center" +|Combined vascular malformations*
! colspan="3" style="background:#4479BA; color: #FFFFFF;" align="center" + |Combined vascular malformations*
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + VM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + VM
|capillary-venous malformation
|capillary-venous malformation
|CVM
|CVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + LM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + LM
|capillary-lymphatic malformation
|capillary-lymphatic malformation
|CLM
|CLM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + AVM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + AVM
|capillary-arteriovenous malformation
|capillary-arteriovenous malformation
|CAVM
|CAVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|LM + VM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |LM + VM
|lymphatic-venous malformation
|lymphatic-venous malformation
|LVM
|LVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + LM + VM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + LM + VM
|capillary-lymphatic-venous malformation
|capillary-lymphatic-venous malformation
|CLVM
|CLVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + LM + AVM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + LM + AVM
|capillary-lymphatic-arteriovenous malformation
|capillary-lymphatic-arteriovenous malformation
|CLAVM
|CLAVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + VM + AVM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + VM + AVM
|capillary-venous-arteriovenous malformation
|capillary-venous-arteriovenous malformation
|CVAVM
|CVAVM
|-
|-
|style="background:#7d7d7d; color: #FFFFFF;" align="center" +|CM + LM + VM + AVM
| style="background:#7d7d7d; color: #FFFFFF;" align="center" + |CM + LM + VM + AVM
|capillary-lymphatic-venous-arteriovenous m.
|capillary-lymphatic-venous-arteriovenous m.
|CLVAVM
|CLVAVM
|-
| colspan="2" style="background:#F5F5F5;" + |<small>'''Adapted from International Society for the Study of Vascular Anomalies'''<ref name="urlClassification | International Society for the Study of Vascular Anomalies">{{cite web |url=http://www.issva.org/classification |title=Classification &#124; International Society for the Study of Vascular Anomalies |format= |work= |accessdate=}}</ref></small>
|}
|}
'''Abbreviations:''' CM:capillary malformation; VM:venous malformation; CVM:capillary venous malformation; LM:lymphatic malformation; CLM:capillary lymphatic malformation; AVM:arteriovenous malformation; CAVM:capillary arteriovenous malformation; LVM:lymphatic venous malformation; CLVM:capillary lymphatic venous malformation; CVAVM:capillary venous arteriovenous malformation; CLVAVM:capillary lymphatic venous arteriovenous malformation.


=Vascular Malformations of Major Named Vessels=
=Vascular Malformations of Major Named Vessels=
{| class="wikitable" style="text-align:centre"
{| class="wikitable" style="text-align:centre"
|+
|+
!style="background:#4479BA; color: #FFFFFF;" align="center" + |Anomalies of major named vessels
! style="background:#4479BA; color: #FFFFFF;" align="center" + |Anomalies of major named vessels
(also known as "channel type" or "truncal" vascular malformations)
(also known as "channel type" or "truncal" vascular malformations)
|-
|-
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*communication (AVF)
*communication (AVF)
*persistence (of embryonal vessel)
*persistence (of embryonal vessel)
|-
| colspan="2" style="background:#7d7d7d; color: #FFFFFF;" + |<small>'''Adapted from International Society for the Study of Vascular Anomalies'''<ref name="urlClassification | International Society for the Study of Vascular Anomalies">{{cite web |url=http://www.issva.org/classification |title=Classification &#124; International Society for the Study of Vascular Anomalies |format= |work= |accessdate=}}</ref></small>
|}
|}
'''Abbreviations:''' AVF:arteriovenous fistula.


=Vascular Malformations associated With other Anomalies=
=Vascular Malformations associated With other Anomalies=
{| class="wikitable" style="text-align:center"
{| class="wikitable" style="text-align:center"
! colspan="3" style="background:#4479BA; color: #FFFFFF;" align="center" +|Vascular malformations associated with other anomalies
! colspan="3" style="background:#4479BA; color: #FFFFFF;" align="center" + |Vascular malformations associated with other anomalies
|-
|-
| colspan="2" |'''Klippel-Trenaunay syndrome*'''
| colspan="2" |'''[[Klippel-Trenaunay syndrome]]*'''
|CM + VM +/-LM + limb overgrowth
|CM + VM +/-LM + limb overgrowth
|-
|-
| colspan="2" |'''Parkes Weber syndrome'''
| colspan="2" |'''[[Parkes Weber syndrome]]'''
|CM + AVF + limb overgrowth
|CM + AVF + limb overgrowth
|-
|-
| colspan="2" |'''Servelle-Martorell syndrome'''
| colspan="2" |'''[[Servelle-Martorell syndrome]]'''
|limb VM + bone undergrowth
|limb VM + bone undergrowth
|-
|-
| colspan="2" |'''Sturge-Weber syndrome'''
| colspan="2" |'''[[Sturge-Weber syndrome]]'''
|facial + leptomeningeal CM + eye anomalies  
|facial + leptomeningeal CM + eye anomalies  
+/-bone and/or soft tissue overgrowth
+/-bone and/or soft tissue overgrowth
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|
|
|-
|-
| colspan="2" |'''Maffucci syndrome'''
| colspan="2" |'''[[Maffucci syndrome]]'''
|VM +/-spindle-cell hemangioma + enchondroma
|VM +/-spindle-cell hemangioma + enchondroma
|-
|-
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|
|
|-
|-
| colspan="2" |'''CLOVES syndrome*'''
| colspan="2" |'''[[CLOVES syndrome]]*'''
|LM + VM + CM +/-AVM+ lipomatous overgrowth
|LM + VM + CM +/-AVM+ lipomatous overgrowth
|-
|-
| colspan="2" |'''Proteus syndrome'''
| colspan="2" |'''[[Proteus syndrome]]'''
|CM, VM and/or LM + asymmetrical somatic overgrowth
|CM, VM and/or LM + asymmetrical somatic overgrowth
|-
|-
|'''Bannayan-Riley-Ruvalcaba sd'''
|'''[[Bannayan-Riley-Ruvalcaba syndrome]]'''
| colspan="2" |lower lip CM + face and neck LM + asymmetry and partial/generalized overgrowth
| colspan="2" |lower lip CM + face and neck LM + asymmetry and partial/generalized overgrowth
|-
| colspan="2" style="background:#7d7d7d; color: #FFFFFF;" + |<small>'''Adapted from International Society for the Study of Vascular Anomalies'''<ref name="urlClassification | International Society for the Study of Vascular Anomalies">{{cite web |url=http://www.issva.org/classification |title=Classification &#124; International Society for the Study of Vascular Anomalies |format= |work= |accessdate=}}</ref></small>
|}
|}
==Provisionally unclassified vascular anomalies==
'''Abbreviations:''' CM:capillary malformation; VM:venous malformation; LM:lymphatic malformation; AVM:arteriovenous malformation; AVF:arteriovenous fistula; CLOVES:congenital lipomatous overgrowth, vascular malformations, epidermal nevi, skeletal/scoliosis and spinal abnormalities; M-CM:macrocephaly-capillary malformation; MCAP:megalencephaly-capillary malformation-polymicrogyria; MICCAP:microcephaly-capillary malformation.
===Intramuscular hemangioma===
 
* Characterized by [[benign]] proliferation of [[vascular]] channels. Majority of [[lesions]] occur in [[subcutaneous]] [[adipose]] [[tissues]], followed by [[muscles]]. [[Thigh]] and [[calf]] are most common sites of occurrence. Majority of the [[lesions]] are [[asymptomatic]]. Typical clinical presentation includes chronic pain and swelling that both may increase with exercise of affected [[muscle]] due to increased [[blood]] flow. Other clinical manifestations may include pulsations, discoloration over the [[lesion]], [[lesion]] enlargement when in dependent position, increased temperature, [[muscle contracture]], tenderness, and [[muscle]] weakness and fatigue.<ref name="pmid25028288">{{cite journal |vauthors=Wang CS, Wu PK, Chiou HJ, Chen CF, Chen WM, Liu CL, Chen TH |title=Nonpalpable intramuscular hemangioma treated with hookwire localization and excision |journal=J Chin Med Assoc |volume=77 |issue=8 |pages=426–9 |date=August 2014 |pmid=25028288 |doi=10.1016/j.jcma.2014.02.017 |url=}}</ref><ref name="pmid25728120">{{cite journal |vauthors=Doddanna SJ, Dawar G, Rallan NS, Agarwal M |title=Intramuscular cavernous hemangioma: a rare entity in the buccinator muscle |journal=Indian J Dent Res |volume=25 |issue=6 |pages=813–5 |date=2014 |pmid=25728120 |doi=10.4103/0970-9290.152211 |url=}}</ref><ref name="pmid23845293">{{cite journal |vauthors=Righini CA, Berta E, Atallah I |title=Intramuscular cavernous hemangioma arising from the masseter muscle |journal=Eur Ann Otorhinolaryngol Head Neck Dis |volume=131 |issue=1 |pages=57–9 |date=February 2014 |pmid=23845293 |doi=10.1016/j.anorl.2013.03.003 |url=}}</ref><ref name="pmid25590509">{{cite journal |vauthors=Alami B, Lamrani Y, Addou O, Boubbou M, Kamaoui I, Maaroufi M, Sqalli N, Tizniti S |title=Presumptive intramuscular hemangioma of the masseter muscle |journal=Am J Case Rep |volume=16 |issue= |pages=16–9 |date=January 2015 |pmid=25590509 |pmc=4298281 |doi=10.12659/AJCR.890776 |url=}}</ref><ref name="pmid15155443">{{cite journal |vauthors=Brown RA, Crichton K, Malouf GM |title=Intramuscular haemangioma of the thigh in a basketball player |journal=Br J Sports Med |volume=38 |issue=3 |pages=346–8 |date=June 2004 |pmid=15155443 |pmc=1724833 |doi= |url=}}</ref><ref name="pmid28507959">{{cite journal |vauthors=Patnaik S, Kumar P, Nayak B, Mohapatra N |title=Intramuscular Arteriovenous Hemangioma of Thigh: A Case Report and Review of Literature |journal=J Orthop Case Rep |volume=6 |issue=5 |pages=20–23 |date=2016 |pmid=28507959 |pmc=5404154 |doi=10.13107/jocr.2250-0685.612 |url=}}</ref>
===Klippel-Trenaunay syndrome===
* Intramuscular hemangiomas may be associated with [[Kasabach-Merritt syndrome]] characterized by [[thrombocytopenia]] and/or consumptive [[coagulopathy]]. This [[lesion]] may also lead to functional impairment, [[congestive cardiac failure]] due to arteriovenous shunting, pressure symptoms, [[skin]] [[necrosis]] and may also erode [[bone]].<ref name="pmid15155443" />
* First described by Klippel and Trenaunay in 1900, this [[congenital]] syndrome is characterized by presence of [[capillary malformations]], [[venous malformations]], and [[soft tissues]] and [[bone]] [[hypertrophy]]. [[Lymphatic malformations]] may or may not be present. [[Capillary malformations]] typically present in form of [[capillary hemangioma]] and can occur anywhere on the [[body]] while [[venous]] and [[lymphatic malformations]], and [[soft tissue]] and [[bone]] [[hypertrophy]] usually involves the [[extremities]].<ref name="pmid26451379">{{cite journal |vauthors=Abdolrahimzadeh S, Scavella V, Felli L, Cruciani F, Contestabile MT, Recupero SM |title=Ophthalmic Alterations in the Sturge-Weber Syndrome, Klippel-Trenaunay Syndrome, and the Phakomatosis Pigmentovascularis: An Independent Group of Conditions? |journal=Biomed Res Int |volume=2015 |issue= |pages=786519 |date=2015 |pmid=26451379 |pmc=4588354 |doi=10.1155/2015/786519 |url=}}</ref><ref name="pmid25427442">{{cite journal |vauthors=Withana M, Rodrigo C, Shivanthan MC, Warnakulasooriya S, Wimalachandra M, Gooneratne L, Rajapakse S |title=Klippel-Trenaunay syndrome presenting with acanthocytosis and splenic and retroperitoneal lymphangioma: a case report |journal=J Med Case Rep |volume=8 |issue= |pages=390 |date=November 2014 |pmid=25427442 |pmc=4289367 |doi=10.1186/1752-1947-8-390 |url=}}</ref><ref name="pmid25293688">{{cite journal |vauthors=Ricks CB, Grandhi R, Ducruet AF |title=Klippel-Trenaunay syndrome and cavernous malformations |journal=BMJ Case Rep |volume=2014 |issue= |pages= |date=October 2014 |pmid=25293688 |pmc=4187537 |doi=10.1136/bcr-2014-207486 |url=}}</ref><ref name="pmid28458832">{{cite journal |vauthors=Baba A, Yamazoe S, Okuyama Y, Shimizu K, Kobashi Y, Nozawa Y, Munetomo Y, Mogami T |title=A rare presentation of Klippel-Trenaunay syndrome with bilateral lower limbs |journal=J Surg Case Rep |volume=2017 |issue=2 |pages=rjx024 |date=February 2017 |pmid=28458832 |pmc=5400491 |doi=10.1093/jscr/rjx024 |url=}}</ref><ref name="pmid27921060">{{cite journal |vauthors=Tetangco EP, Arshad HM, Silva R |title=Klippel-Trenaunay Syndrome of the Rectosigmoid Colon Presenting as Severe Anemia |journal=ACG Case Rep J |volume=3 |issue=4 |pages=e161 |date=August 2016 |pmid=27921060 |pmc=5126491 |doi=10.14309/crj.2016.134 |url=}}</ref>
* [[Etiology]] and [[pathophysiology]] are not clearly defined but majority of the [[lesions]] are congenital while a one fifth may be associated with trauma.<ref name="pmid24427416">{{cite journal |vauthors=Wierzbicki JM, Henderson JH, Scarborough MT, Bush CH, Reith JD, Clugston JR |title=Intramuscular hemangiomas |journal=Sports Health |volume=5 |issue=5 |pages=448–54 |date=September 2013 |pmid=24427416 |pmc=3752185 |doi=10.1177/1941738112470910 |url=}}</ref>
* Clinical manifestations are unilateral in 85% of the cases and may include localized pain and discomfort, leg length discrepancy due to [[hemihypertrophy]], [[developmental delay]], limb abnormalities such as [[polydactyly]], macrodactyly, [[syndactyly]], [[thrombophlebitis]], [[osteomyelitis]], pathological [[fractures]], [[heart failure]], [[erysipelas]], [[venous thrombosis]] due to [[malformations]], [[pulmonary embolism]], [[gastrointestinal]] bleeding due to venous overload in the [[internal iliac vein]] and [[ophthalmic]] abnormalities such as [[telangiectasia]], orbital varix, [[strabismus]], oculosympathetic palsy, [[Marcus Gunn pupil|Marcus-Gunn pupil]], iris coloboma and heterochromia, [[cataracts]], persistent fetal vasculature and [[varicosities]].<ref name="pmid28458832" /><ref name="pmid27921060" /><ref name="pmid25293688" /><ref name="pmid29930667">{{cite journal |vauthors=Chagas CAA, Pires LAS, Babinski MA, Leite TFO |title=Klippel-Trenaunay and Parkes-Weber syndromes: two case reports |journal=J Vasc Bras |volume=16 |issue=4 |pages=320–324 |date=2017 |pmid=29930667 |pmc=5944310 |doi=10.1590/1677-5449.005417 |url=}}</ref>
* [[MRI]] is the [[diagnostic]] study of choice although [[X-RAY]] and [[ultrasound]] may be used as initial studies. Treatment is generally not indicated for [[asymptomatic]] [[lesions]]. Management options for [[symptomatic]], complicated [[lesions]] and for cosmetic reasons may include [[laser ablation]], systemic [[corticosteroids]], [[cryotherapy]], [[embolization]], [[radiation]], compression [[sclerotherapy]], and [[surgical excision]] although surgical excision is usually treatment of choice in majority of the cases.<ref name="pmid24427416" /><ref name="pmid15155443" /><ref name="pmid28507959" /><ref name="pmid25028288"></ref><ref name="pmid25728120"></ref><ref name="pmid23845293"></ref><ref name="pmid25590509"></ref>
* [[Etiology]] and [[pathogenesis]] have not been established yet. Some suggestions include PIK3CA mutations, [[polygenic]] [[inheritance]], VG5Q mutation and obstruction of the [[venous]] system.<ref name="pmid26451379" /><ref name="pmid28458832" /><ref name="pmid29930667" />
* [[Diagnosis]] can be made on clinical manifestations and can be confirmed by [[Doppler ultrasound]] and [[magnetic resonance angiography]]. Management depends on clinical manifestations.<ref name="pmid28458832" /><ref name="pmid29930667" /><ref name="pmid25293688" /><ref name="pmid28458832" />
For more information on Klippel-Trenaunay syndrome, [[Klippel-Trenaunay-Weber syndrome#Klippel-Trenaunay-Weber syndrome|click here]]
 
===Parkes Weber syndrome===
* Characterized by a [[cutaneous]] flush with underlying multiple micro-AVFs ([[Arteriovenous fistula|arteriovenous fistulas]]), in association with [[soft tissue]] and skeletal hypertrophy of the affected limb. Clinical Presentation enlarged [[arteries]] and [[veins]], [[capillary]] or [[venous]] [[malformations]], [[cutaneous]] blush, [[arteriovenous fistulas]], and enlargement of [[limb]].
* Mutation in the RASA1 gene has been found to be associated with this [[syndrome]].
For more information on [[Parkes Weber syndrome]], [[Parkes Weber syndrome#Parkes Weber syndrome|click here]].
 
===Servelle-Martorell syndrome===
* Also called phlebectatic osteohypoplastic angiodysplasia, this rare [[syndrome]] is characterized by [[venous malformations]] such as abnormal location of [[vein]], partial or complete absence of valves, and/or venous [[hypoplasia]] or [[aplasia]] and undergrowth of [[bone]]. These abnormalities may also be associated with limb hypertrophy and arterial malformations.<ref name="pmid18454870">{{cite journal |vauthors=Karuppal R, Raman RV, Valsalan BP, Gopakumar Ts, Kumaran CM, Vasu CK |title=Servelle-Martorell syndrome with extensive upper limb involvement: a case report |journal=J Med Case Rep |volume=2 |issue= |pages=142 |date=May 2008 |pmid=18454870 |pmc=2394530 |doi=10.1186/1752-1947-2-142 |url=}}</ref>
* Clinical manifestations may include [[cutaneous]] compressible [[lesions]] due to [[malformations]], [[cellulitis]], [[lesion]] limb shortening, [[joint]] and [[soft tissue]] pain and swelling, tortuous [[limbs]], reduced [[muscle]] mass, [[venous thrombosis]], consumption [[coagulopathy]], pathological [[fractures]] and [[bone]] tenderness.<ref name="pmid18454870" />
* Combination of clinical and [[radiological]] findings is used to form the [[diagnosis]], [[MRI]] can assess the involvement and extent of [[lesions]]. Treatment is mainly conservative with [[surgery]] being used in some cases to excise and/or correct [[malformations]].<ref name="pmid18454870" /><ref name="pmid6284617">{{cite journal |vauthors=Langer M, Langer R |title=[Radiologic aspects of the congenital arteriovenous malformations, Klippel-Trenaunay type, and Servelle-Martorell type (author's transl)] |language=German |journal=Rofo |volume=136 |issue=5 |pages=577–82 |date=May 1982 |pmid=6284617 |doi=10.1055/s-2008-1056105 |url=}}</ref>
 
===Sturge-Weber syndrome===
* [[Congenital]] [[syndrome]] characterized by [[capillary malformations]] involving [[face]] and laptomeninges and [[eye]] abnormalities. There may also be bone and/or overgrowth.
* Clinical manifestations may include [[seizures]], [[port-wine stain]] on the forehead and upper [[eyelid]] of one side of the [[face]],  [[muscle]] weakness, [[developmental delays]] and [[mental retardation]], [[glaucoma]], and [[buphthalmos]].
* Associated with [[mutations]] in GNAQ [[gene]] that encodes for members of [[G protein]] family.
For more information on [[Sturge-Weber syndrome]], [[Sturge-Weber syndrome#Sturge-Weber syndrome|click here]].


===Angiokeratoma===
===Maffucci syndrome===
* A [[muco-cutaneous]] [[vascular]] [[lesion]] with wart-like papular appearance characterized by dilated [[capillaries]] in the [[dermis]] and [[hyperkeratotis]] of the overlying [[epidermis]]. Clinically it may manifest as solitary or multiple hyperkeratotic papules that may be localized or generalized, most typically on [[scrotum]], [[thighs]], lower extremity, [[abdomen]], [[trunk]], [[tongue]], [[penis]] and [[labia majora]]. Majority of the [[lesions]] are [[asymptomatic]] but some may ulcerate and/or bleed.<ref name="pmid25100920">{{cite journal |vauthors=Hussein RS, Kfoury H, Al-Faky YH |title=Eyelid angiokeratoma |journal=Middle East Afr J Ophthalmol |volume=21 |issue=3 |pages=287–8 |date=2014 |pmid=25100920 |pmc=4123288 |doi=10.4103/0974-9233.134702 |url=}}</ref><ref name="pmid16988295">{{cite journal |vauthors=Trickett R, Dowd H |title=Angiokeratoma of the scrotum: a case of scrotal bleeding |journal=Emerg Med J |volume=23 |issue=10 |pages=e57 |date=October 2006 |pmid=16988295 |pmc=2579622 |doi=10.1136/emj.2006.038745 |url=}}</ref><ref name="pmid26155544">{{cite journal |vauthors=Chowdappa V, Narasimha A, Bhat A, Masamatti SS |title=Solitary Angiokeratoma: Report of Two Uncommon Cases |journal=J Clin Diagn Res |volume=9 |issue=5 |pages=WD01–2 |date=May 2015 |pmid=26155544 |pmc=4484136 |doi=10.7860/JCDR/2015/12163.5946 |url=}}</ref>
* A rare [[disorder]] characterized by presence of [[venous malformations]] associated with multiple [[enchondromas]], benign [[cartilage]]-forming [[tumors]], and multiple [[soft tissue]] [[hemangiomas]], and [[lymphangiomas]]. These benign [[tumors]] have tendency to undergo [[malignant]] [[transformation]] in [[Maffucci syndrome]]. People with [[Maffucci syndrome]] are also at increased risk of developing other [[malignant]] [[tumors]] such as [[glioma]], [[glioblastoma]], [[acute myeloid leukemia]], intrahepatic cholangiocarcinomas, [[hepatocellular carcinoma]], [[pancreatic]], and [[breast]] [[malignancies]]. Clinical manifestations depend on the coexisting [[lesions]].<ref name="pmid25777744">{{cite journal |vauthors=McCarthy CM, Blecher H, Reich S |title=A case of myelopathy because of enchondromas from Maffucci syndrome with successful surgical treatment |journal=Spine J |volume=15 |issue=6 |pages=e15–9 |date=June 2015 |pmid=25777744 |doi=10.1016/j.spinee.2015.03.006 |url=}}</ref><ref name="pmid26628708">{{cite journal |vauthors=Tsao YP, Tsai CY, Chen WS |title=Maffucci Syndrome |journal=J. Rheumatol. |volume=42 |issue=12 |pages=2434–5 |date=December 2015 |pmid=26628708 |doi=10.3899/jrheum.150216 |url=}}</ref><ref name="pmid26920730">{{cite journal |vauthors=Prokopchuk O, Andres S, Becker K, Holzapfel K, Hartmann D, Friess H |title=Maffucci syndrome and neoplasms: a case report and review of the literature |journal=BMC Res Notes |volume=9 |issue= |pages=126 |date=February 2016 |pmid=26920730 |pmc=4769492 |doi=10.1186/s13104-016-1913-x |url=}}</ref>
* It may be classified into following entities:<ref name="pmid26155544"></ref>
* [[Mutations]] in [[Isocitrate dehydrogenase|isocitrate dehydrogenase 1]] (IDH1) and [[Isocitrate dehydrogenase|isocitrate dehydrogenase 2]] (IDH2), [[enzymes]] involved in metabolism of isocitrate and α-ketoglutarate, and [[TP53]], a [[cell-cycle]] regulator, have been found in [[tumors]] in [[Maffucci syndrome]].<ref name="pmid24344754">{{cite journal |vauthors=Moriya K, Kaneko MK, Liu X, Hosaka M, Fujishima F, Sakuma J, Ogasawara S, Watanabe M, Sasahara Y, Kure S, Kato Y |title=IDH2 and TP53 mutations are correlated with gliomagenesis in a patient with Maffucci syndrome |journal=Cancer Sci. |volume=105 |issue=3 |pages=359–62 |date=March 2014 |pmid=24344754 |pmc=4317937 |doi=10.1111/cas.12337 |url=}}</ref><ref name="pmid22057234">{{cite journal |vauthors=Pansuriya TC, van Eijk R, d'Adamo P, van Ruler MA, Kuijjer ML, Oosting J, Cleton-Jansen AM, van Oosterwijk JG, Verbeke SL, Meijer D, van Wezel T, Nord KH, Sangiorgi L, Toker B, Liegl-Atzwanger B, San-Julian M, Sciot R, Limaye N, Kindblom LG, Daugaard S, Godfraind C, Boon LM, Vikkula M, Kurek KC, Szuhai K, French PJ, Bovée JV |title=Somatic mosaic IDH1 and IDH2 mutations are associated with enchondroma and spindle cell hemangioma in Ollier disease and Maffucci syndrome |journal=Nat. Genet. |volume=43 |issue=12 |pages=1256–61 |date=November 2011 |pmid=22057234 |pmc=3427908 |doi=10.1038/ng.1004 |url=}}</ref>
** Fordyce’s angiokeratoma (arising on the genitals)
* [[Patients]] should be evaluated to check for [[malignant]] [[transformation]]. Some recommend [[CT scans]] and [[PET scans]] at regular intervals.<ref name="pmid26920730" /><ref name="pmid26628708" /><ref name="pmid25537758">{{cite journal |vauthors=Al-Katib S, Al-Faham Z, Grant P, Palka JC |title=The Appearance of Maffucci Syndrome on 18F-FDG PET/CT |journal=J Nucl Med Technol |volume=43 |issue=2 |pages=131–2 |date=June 2015 |pmid=25537758 |doi=10.2967/jnmt.114.146480 |url=}}</ref><ref name="pmid26920730" />
** Mibelli’s angiokeratoma (dorsum of toes and fingers)
For more information on [[Maffucci syndrome]], [[Maffucci syndrome#Maffucci syndrome|click here]].
** Angiokeratoma circumscriptum naeviforme (unilateral large keratotic plaques)
** Angiokeratoma corporis diffusum (ACD) (generalized [[lesions]] between umbilicus and the knee)
* Angiokeratomas are more prevalent among [[males]] as compared to [[females]]. Increased [[venous]] pressure and [[radiation]] therapy have been cited as possible causes. Angiokeratomas have been associated with [[enzyme]] deficiencies such as  alpha-galactosidase A ([[Fabry disease]]), α-fucosidase (fucosidosis), neuraminidase (sialodosis), aspartyl glycosaminase (aspartyl glucosaminuria), β-mannosidase (β- mannosidosis), α-N-acetyl galactosaminidase (Kansaki disease), and β-galactosidase (adult onset GM1 gangliosidosis).<ref name="pmid26155544"></ref><ref name="pmid25100920"></ref><ref name="pmid16988295"></ref><ref name="pmid26312700">{{cite journal |vauthors=Ghosh SK, Ghosh S, Agarwal M |title=Multiple giant angiokeratoma of Fordyce on the shaft of the penis masquerading as keratoacanthoma |journal=An Bras Dermatol |volume=90 |issue=3 Suppl 1 |pages=150–2 |date=2015 |pmid=26312700 |pmc=4540534 |doi=10.1590/abd1806-4841.20153876 |url=}}</ref><ref name="pmid19468654">{{cite journal |vauthors=Rees R, Freeman A, Malone P, Garaffa G, Muneer A, Minhas S |title=Case study: the surgical management of angiokeratoma resulting from radiotherapy for penile cancer |journal=ScientificWorldJournal |volume=9 |issue= |pages=339–42 |date=May 2009 |pmid=19468654 |pmc=5823195 |doi=10.1100/tsw.2009.23 |url=}}</ref>
* The [[diagnosis]] is mainly clinical but [[biopsy]] may be required. Associated [[enzyme]] deficiencies and systemic disorders must be ruled out. Treatment is generally not indicated but if so required then [[excision]], [[electrocautery]], [[cryotherapy]], or [[laser ablations]] are the options.<ref name="pmid25100920"></ref><ref name="pmid19468654"></ref><ref name="pmid26155544"></ref><ref name="pmid25118768">{{cite journal |vauthors=Vijay MK, Arava S |title=Solitary angiokeratoma of tongue: a rare entity clinically mistaken as a malignant tumor |journal=Indian J Pathol Microbiol |volume=57 |issue=3 |pages=510–1 |date=2014 |pmid=25118768 |doi=10.4103/0377-4929.138810 |url=}}</ref><ref name="pmid26312700"></ref>


===Sinusoidal hemangioma===
===CLOVES syndrome===
* A variant of [[cavernous hemangioma]] characterized histopathologically by presence of dilated thin-walled [[vascular]] channels, that vary in size, exhibiting nodular proliferation with sinusoidal arrangement.  [[Pseudopapillary]] structures may also be present. Clinically majority of the [[lesions]] manifest in [[female]] [[adults]] as single, well-defined, painless, [[subcutaneous]] nodule with bluish color. Most frequent locations are [[trunk]], [[extremities]] and [[breasts]]. Painless swelling is the most common [[patient]] complaint.<ref name="pmid24250102">{{cite journal |vauthors=Halawar SS, Venugopal R, Varsha B, Kavya B |title=Intramuscular sinusoidal hemangioma with Masson's lesion |journal=J Oral Maxillofac Pathol |volume=17 |issue=2 |pages=315–7 |date=May 2013 |pmid=24250102 |pmc=3830250 |doi=10.4103/0973-029X.119762 |url=}}</ref><ref name="pmid21892538">{{cite journal |vauthors=Ciurea M, Ciurea R, Popa D, Pârvănescu H, Marinescu D, Vrabete M |title=Sinusoidal hemangioma of the arm: case report and review of literature |journal=Rom J Morphol Embryol |volume=52 |issue=3 |pages=915–8 |date=2011 |pmid=21892538 |doi= |url=}}</ref>
* CLOVES is an acronym for [[congenital]] lipomatous overgrowth, [[vascular malformations]], [[epidermal nevi]], skeletal and spinal anomalies. [[Vascular malformations]] in this [[syndrome]] include [[venous]], [[capillary]] and [[lymphatic]] [[malformations]] with or without combined [[arteriovenous malformations]]. [[Pulmonary thromboembolism]] and [[respiratory]] failure are the cause of [[mortality]] in majority of the [[patients]]. Lipomatous and vascular abnormalities are often segmental and [[asymmetric]] in distribution and present typically on [[chest]] and [[abdominal wall]].<ref name="pmid25044986">{{cite journal |vauthors=Emrick LT, Murphy L, Shamshirsaz AA, Ruano R, Cassady CI, Liu L, Chang F, Sutton VR, Li M, Van den Veyver IB |title=Prenatal diagnosis of CLOVES syndrome confirmed by detection of a mosaic PIK3CA mutation in cultured amniocytes |journal=Am. J. Med. Genet. A |volume=164A |issue=10 |pages=2633–7 |date=October 2014 |pmid=25044986 |pmc=4496426 |doi=10.1002/ajmg.a.36672 |url=}}</ref><ref name="pmid25400966">{{cite journal |vauthors=Sarici D, Akin MA, Kurtoglu S, Tubas F, Sarici SU |title=A Neonate with CLOVES Syndrome |journal=Case Rep Pediatr |volume=2014 |issue= |pages=845074 |date=2014 |pmid=25400966 |pmc=4221976 |doi=10.1155/2014/845074 |url=}}</ref><ref name="pmid20537357">{{cite journal |vauthors=Alomari AI, Burrows PE, Lee EY, Hedequist DJ, Mulliken JB, Fishman SJ |title=CLOVES syndrome with thoracic and central phlebectasia: increased risk of pulmonary embolism |journal=J. Thorac. Cardiovasc. Surg. |volume=140 |issue=2 |pages=459–63 |date=August 2010 |pmid=20537357 |doi=10.1016/j.jtcvs.2010.04.023 |url=}}</ref><ref name="pmid25709171">{{cite journal |vauthors=Gopal B, Keshava SN, Selvaraj D |title=A rare newly described overgrowth syndrome with vascular malformations-Cloves syndrome |journal=Indian J Radiol Imaging |volume=25 |issue=1 |pages=71–3 |date=2015 |pmid=25709171 |pmc=4329693 |doi=10.4103/0971-3026.150166 |url=}}</ref>
* Abnormalities of [[vasculogenesis]] and [[angiogenesis]] have been proposed as possible [[pathogenesis]] but it is not well-established.<ref name="pmid21892538"></ref>
* Clinical and [[imaging]] findings may include swellings due to lipomatous growths, [[skin]] discoloration, [[Port-wine stain|port wine stain]], bilateral [[epidermal nevi]],leg length discrepancy, developmental limb anomalies such as increased gap between the first and second toes, [[hemorrhage]], [[seizures]], [[ascites]], [[pleural effusions]], [[hypotension]], bilateral multicystic [[venous]] and [[lymphatic]] [[malformations]], [[chest]] wall [[venous]] dilatation, multiple [[congenital]] [[hemangiomas]], asymmetric [[septal hypertrophy]], [[renal]] hypoplasia, dislocated [[knees]], [[scoliosis]], and [[neural tube defect]].<ref name="pmid25044986" /><ref name="pmid25709171" /><ref name="pmid20537357" />
* Combination of clinical manifestations and histopathological features is used for [[diagnosis]]. [[Surgery]] (wide excision of tumor) is the treatment of choice if treatment is required.<ref name="pmid21892538"></ref><ref name="pmid26729822">{{cite journal |vauthors=Konda P, Bavle RM, Makarla S, Muniswamappa S |title=Intramuscular sinusoidal haemangioma with secondary Masson's phenomenon |journal=BMJ Case Rep |volume=2016 |issue= |pages= |date=January 2016 |pmid=26729822 |pmc=4716435 |doi=10.1136/bcr-2013-201457 |url=}}</ref>
* Activating mutations in PICK3CA [[gene]] that encodes part of PI3K has been thought to be associated with this [[syndrome]]. These mutations may help enable the cells to grow independent of [[growth factors]].<ref name="pmid25044986" /><ref name="pmid25400966" /><ref name="pmid22658544">{{cite journal |vauthors=Kurek KC, Luks VL, Ayturk UM, Alomari AI, Fishman SJ, Spencer SA, Mulliken JB, Bowen ME, Yamamoto GL, Kozakewich HP, Warman ML |title=Somatic mosaic activating mutations in PIK3CA cause CLOVES syndrome |journal=Am. J. Hum. Genet. |volume=90 |issue=6 |pages=1108–15 |date=June 2012 |pmid=22658544 |pmc=3370283 |doi=10.1016/j.ajhg.2012.05.006 |url=}}</ref>
* This [[syndrome]] can be detected prenatally and its manifestations have been identified on prenatal [[ultrasound]] and fetal [[MRI]]. Treatment options include supportive management, surgical debulking and scletherapy but treatment is often complicated by severity of the disease resulting in [[anemia]], [[coagulopathy]] and poor [[wound healing]].<ref name="pmid25044986" /><ref name="pmid25400966" />


===Acral arteriovenous "tumour"===
===Proteus syndrome===
* [[Congenital]] or acquired lesion manifesting clinically as [[asymptomatic]] mass or may present with pulsatile swelling, headache, localized throbbing pain, [[tinnitus]] and bleeding. Histopathologically they are characterized by [[arterio-venous]] connection without connecting [[capillary]] with or without intracranial component. The [[lesion]] derived its name from its acral distribution.<ref name="pmid25624933">{{cite journal |vauthors=Gupta R, Kayal A |title=Scalp arteriovenous malformations in young |journal=J Pediatr Neurosci |volume=9 |issue=3 |pages=263–6 |date=2014 |pmid=25624933 |pmc=4302550 |doi=10.4103/1817-1745.147587 |url=}}</ref><ref name="pmid29492122">{{cite journal |vauthors=Özkara E, Özbek Z, Özdemir AÖ, Arslantaş A |title=Misdiagnosed Case of Scalp Arteriovenous Malformation |journal=Asian J Neurosurg |volume=13 |issue=1 |pages=59–61 |date=2018 |pmid=29492122 |pmc=5820896 |doi=10.4103/1793-5482.181137 |url=}}</ref>
* [[Congenital]] [[syndrome]] characterized by asymmetric overgrowth of multiple [[tissues]] in [[limbs]], [[hamartomas]] and [[vascular]] [[lesions]] such as [[capillary malformations]], [[venous malformations]], [[lymphatic malformations]]. Cerebriform connective tissue nevi, a [[pathognomonic]] [[lesion]] if present alone, are helpful in diagnosing [[Proteus syndrome]]. It may affect multiple [[organs]] such as [[eyes]], [[spleen]], [[liver]], [[thymus]], [[intestine]], and [[lungs]], and may cause facial dysmorphia. Some [[benign]] and [[malignant]] [[neoplasms]] such as testicular papillary adenocarcinoma and [[mesothelioma]].<ref name="pmid29166516">{{cite journal |vauthors=Rocha RCC, Estrella MPS, Amaral DMD, Barbosa AM, Abreu MAMM |title=Proteus syndrome |journal=An Bras Dermatol |volume=92 |issue=5 |pages=717–720 |date=2017 |pmid=29166516 |pmc=5674710 |doi=10.1590/abd1806-4841.20174496 |url=}}</ref><ref name="pmid28377973">{{cite journal |vauthors=El-Sobky TA, Elsayed SM, El Mikkawy DM |title=Orthopaedic manifestations of Proteus syndrome in a child with literature update |journal=Bone Rep |volume=3 |issue= |pages=104–108 |date=December 2015 |pmid=28377973 |pmc=5365241 |doi=10.1016/j.bonr.2015.09.004 |url=}}</ref><ref name="pmid25377688">{{cite journal |vauthors=Hannoush H, Sachdev V, Brofferio A, Arai AE, LaRocca G, Sapp J, Sidenko S, Brenneman C, Biesecker LG, Keppler-Noreuil KM |title=Myocardial fat overgrowth in Proteus syndrome |journal=Am. J. Med. Genet. A |volume=167A |issue=1 |pages=103–10 |date=January 2015 |pmid=25377688 |pmc=4275354 |doi=10.1002/ajmg.a.36773 |url=}}</ref>
* [[Etiology]] can be classified as following: [[Congenital]], traumatic, infectious and inflammatory and [[familial]].<ref name="pmid25624933"></ref>
* Clinical manifestations and findings may include [[hemihypertrophy]], asymmetry of the limbs, [[scoliosis]], [[subcutaneous]] [[tumors]], [[soft tissues]] [[tumors]] such as [[lipoma]], limb abnormalities such as macrodactyly, hyperpigmented [[lesions]] on [[skin]], [[verrucous epidermal nevi]], [[lung]] diseases, [[pulmonary embolism]], [[venous thrombosis]],  [[glaucoma]], [[strabismus]], [[nystagmus]], pseudopapileudema, [[cardiac defects]] such as ARVC, healed [[myocardial infarctions]], [[cardiomyopathies]], cardiac lipomas, and [[central nervous system]] findings. These findings may be detected [[prenatally]] or at [[birth]] but majority of the [[patients]] present after 6 months of [[birth]].<ref name="pmid29166516" /><ref name="pmid28377973" /><ref name="pmid25377688" /><ref name="pmid24882963">{{cite journal |vauthors=Sarman ZS, Yuksel N, Sarman H, Bayramgurler D |title=Proteus syndrome: report of a case with developmental glaucoma |journal=Korean J Ophthalmol |volume=28 |issue=3 |pages=272–4 |date=June 2014 |pmid=24882963 |pmc=4038735 |doi=10.3341/kjo.2014.28.3.272 |url=}}</ref>
* Although [[diagnosis]] can be made clinically, [[angiography]] is the gold standard [[diagnostic]] modality to [[diagnose]] and define the extent of the [[lesion]]. Management regimen may include [[surgical excision]], [[ligation]] of the supplying [[arteries]], [[embolization]], and intralesional [[sclerosing]] injection.<ref name="pmid29492122"></ref>
* Somatic mutations in AKT1 [[gene]] that encodes [[proteins]] functioning in AKT/PI3K signaling pathway has been proposed to be the cause of this [[syndrome]]. This pathway functions in cell growth, differentiation, and survival.<ref name="pmid25377688" /><ref name="pmid26657992">{{cite journal |vauthors=Lindhurst MJ, Yourick MR, Yu Y, Savage RE, Ferrari D, Biesecker LG |title=Repression of AKT signaling by ARQ 092 in cells and tissues from patients with Proteus syndrome |journal=Sci Rep |volume=5 |issue= |pages=17162 |date=December 2015 |pmid=26657992 |pmc=4675973 |doi=10.1038/srep17162 |url=}}</ref>
* [[Diagnosis]] is based on clinical and [[radiological]] findings and must meet general and specific criteria. Management consists of clinical and psychological assistance. This may include [[orthopedic]] consultation to stop or delay bone growth, [[physical rehabilitation]], [[surgical correction]] of deformities such as [[scoliosis]], [[dermatology]] consultation fro skin [[lesions]], workup and followup for [[vein thrombosis]] and [[pulmonary embolism]], [[intervention]] for [[developmental delay]], and evaluation for associated [[neoplasms]] at regular intervals.<ref name="pmid29166516" /><ref name="pmid22876373">{{cite journal |vauthors=Adam MP, Ardinger HH, Pagon RA, Wallace SE, Bean LJH, Stephens K, Amemiya A, Biesecker LG, Sapp JC |title= |journal= |volume= |issue= |pages= |date= |pmid=22876373 |doi= |url=}}</ref>
For more information about [[Proteus syndrome]], [[Proteus syndrome#Proteus syndrome|click here]].


===Multifocal lymphangioendotheliomatosis with thrombocytopenia / cutaneovisceral angiomatosis with thrombocytopenia (MLT/CAT)===
===Bannayan-Riley-Ruvalcaba syndrome===
* Rare [[congenital]] disorder characterized by proliferation of [[vascular]] channels in multiple [[organs]] associated with [[thrombocytopenia]] of variable degree. [[Lesions]] may manifest themselves on [[skin]], [[gastrointestinal tract]], [[lungs]], [[brain]], [[bone]], [[liver]], [[spleen]] and [[muscles]]. Majority of [[cutaneous]] [[lesions]] present as multiple red to blue papules, plaques, nodules on [[trunk]] and [[extremities]]. [[Gastrointestinal]] bleeding due to multiple [[hemorrhagic]] [[lesions]] is the cause of mortality in majority of the [[patients]]. Similar [[lesions]] in [[brain]] and [[lungs]] may cause severe [[cerebral edema]] and [[pulmonary hemorrhage]].<ref name="pmid26148948">{{cite journal |vauthors=Droitcourt C, Boccara O, Fraitag S, Favrais G, Dupuy A, Maruani A |title=Multifocal Lymphangioendotheliomatosis With Thrombocytopenia: Clinical Features and Response to Sirolimus |journal=Pediatrics |volume=136 |issue=2 |pages=e517–22 |date=August 2015 |pmid=26148948 |doi=10.1542/peds.2014-2410 |url=}}</ref><ref name="pmid22565464">{{cite journal |vauthors=Zegpi MS, Zavala A, del Puerto C, Cárdenas C, González S |title=Newborn with multifocal lymphangioendotheliomatosis with thrombocytopenia |journal=Indian J Dermatol Venereol Leprol |volume=78 |issue=3 |pages=409 |date=2012 |pmid=22565464 |doi=10.4103/0378-6323.95494 |url=}}</ref>
* An overgrowth [[syndrome]] characterized by [[vascular malformations]], macrocephaly, multiple [[benign]] [[neoplasm]] and [[pigmented]] [[lesions]] on the [[skin]]. Speckled [[pigmented]] macules on [[genitalia]] are one of the most significant [[diagnostic]] characteristics. People with this [[syndrome]] may have increased risk of developing [[neoplasms]] in many [[organs]] such as [[thyroid]], [[breasts]], and [[female genital tract]] although it has not been confirmed.<ref name="pmid24474112">{{cite journal |vauthors=Gontijo GM, Pinto CA, Rogatto SR, Cunha IW, Aguiar S, Alves CA |title=Bannayan-Riley-Ruvalcaba syndrome with deforming lipomatous hamartomas in infant--case report |journal=An Bras Dermatol |volume=88 |issue=6 |pages=982–5 |date=2013 |pmid=24474112 |pmc=3900354 |doi=10.1590/abd1806-4841.20132730 |url=}}</ref><ref name="pmid24379037">{{cite journal |vauthors=Peiretti V, Mussa A, Feyles F, Tuli G, Santanera A, Molinatto C, Ferrero GB, Corrias A |title=Thyroid involvement in two patients with Bannayan-Riley-Ruvalcaba syndrome |journal=J Clin Res Pediatr Endocrinol |volume=5 |issue=4 |pages=261–5 |date=2013 |pmid=24379037 |pmc=3890226 |doi=10.4274/Jcrpe.984 |url=}}</ref><ref name="pmid26157835">{{cite journal |vauthors=Sagi SV, Ballard DD, Marks RA, Dunn KR, Kahi CJ |title=Bannayan Ruvalcaba Riley Syndrome |journal=ACG Case Rep J |volume=1 |issue=2 |pages=90–2 |date=January 2014 |pmid=26157835 |pmc=4435287 |doi=10.14309/crj.2014.11 |url=}}</ref>  
* Disease may manifest without [[cutaneous]] involvement or [[thrombocytopenia]]. [[Biopsy]] typically reveals proliferation of well differentiated [[vascular]] channels with intravascular [[papillary]] structure and thrombi, sometimes with hobnail appearance of lining [[endothelial cells]].<ref name="pmid26148948"></ref><ref name="pmid22565464"></ref>
* Typical manifestations and findings may include  multiple [[lipomas]], [[hemangiomas]], intestinal hamartomatous polyposis, [[vascular malformations]] such as [[arteriovenous malformations]] and [[capillary malformations]], [[developmental delay]], macrocephaly (>97 percentile), [[penile]] [[pigmented]] macules, thyroid abnormalities such as [[multinodular goiter]], [[thyroid]] [[adenoma]], differentiated non-medullary thyroid cancer and [[Hashimoto's thyroiditis|Hashimoto’s thyroiditis]], high-arched palate, protuberant frontal bone, [[hypertelorism]], [[strabismus]], [[macrosomia]], [[hypotonia]], joint hyperextensibility, [[hypoglycemia]], [[convulsions]], [[café-au-lait spots]], prominent forehead, malar hypoplasia and [[micrognathia]].<ref name="pmid24474112" /><ref name="pmid24379037" /><ref name="pmid26157835" />
* [[Biopsy]] followed by histopathological and [[immunohistochemical]] are required for [[diagnosis]]. Management is not well-established and disorder has a poor [[prognosis]] with high mortality. Recently [[sirolimus]] and [[bevacizumab]] have been used to treat this diorder with some success.<ref name="pmid26148948"></ref><ref name="pmid22565464"></ref><ref name="pmid19101995">{{cite journal |vauthors=Kline RM, Buck LM |title=Bevacizumab treatment in multifocal lymphangioendotheliomatosis with thrombocytopenia |journal=Pediatr Blood Cancer |volume=52 |issue=4 |pages=534–6 |date=April 2009 |pmid=19101995 |doi=10.1002/pbc.21860 |url=}}</ref><ref name="pmid27282436">{{cite journal |vauthors=Lanöel A, Torres Huamani AN, Feliú A, Sala MJ, Alvarez M, Cervini AB |title=Multifocal Lymphangioendotheliomatosis with Thrombocytopenia: Presentation of Two Cases Treated with Sirolimus |journal=Pediatr Dermatol |volume=33 |issue=4 |pages=e235–9 |date=July 2016 |pmid=27282436 |doi=10.1111/pde.12879 |url=}}</ref>
* [[Mutations]] in PTEN [[gene]] have been thought to be the cause. This [[gene]] encodes an [[enzyme]] that acts as [[tumor]] suppressor by stopping [[cell division]] and inducing [[apoptosis]]. Both [[Autosomal dominant|autosomal-dominant]] transmission and sporadic occurrence have been reported.<ref name="pmid24474112" />
* [[Diagnosis]] is based on clinical findings, the most important of these findings being [[penile pigmented maculae]], [[hamartomatous intestinal polyposis]] and macrocephaly. Management consists of psycho-social counseling and treatment of manifestations such as [[surgical]] and [[dermatological]] interventions, spinal stimulation for intractable gastrointestinal pain and screening for malignancies associated with PTEN mutations such as annual [[thyroid]] [[ultrasound]] and [[mammography]].<ref name="pmid24474112" /><ref name="pmid26157835" />
For more information on Bannayan-Riley-Ruvalcaba syndrome, [[Bannayan-Zonana syndrome#Bannayan-Zonana syndrome|click here]].


===Fibro adipose vascular anomaly (FAVA)===
===CLAPO syndrome===
* [[Vascular]] [[disorder]] typically manifesting as infiltration of [[muscles]] by fibrofatty tissues, atypical [[venodilation]] associated with localized pain, and contracture of the affected [[muscles]]. Majority of the [[lesions]] involve [[calf]] [[muscles]] and may present as painful mass, [[contracture]] of the [[extremity]], and decreased dorsiflexion at ankle joint. [[Skin]] is not typically involved. Histological studies demonstrates fibrous and [[adipose tissue]] and congregations of [[venous]] channels with abnormal [[lymphatic]] component.<ref name="pmid25298836">{{cite journal |vauthors=Fernandez-Pineda I, Marcilla D, Downey-Carmona FJ, Roldan S, Ortega-Laureano L, Bernabeu-Wittel J |title=Lower Extremity Fibro-Adipose Vascular Anomaly (FAVA): A New Case of a Newly Delineated Disorder |journal=Ann Vasc Dis |volume=7 |issue=3 |pages=316–9 |date=2014 |pmid=25298836 |pmc=4180696 |doi=10.3400/avd.cr.14-00049 |url=}}</ref><ref name="pmid24322574">{{cite journal |vauthors=Alomari AI, Spencer SA, Arnold RW, Chaudry G, Kasser JR, Burrows PE, Govender P, Padua HM, Dillon B, Upton J, Taghinia AH, Fishman SJ, Mulliken JB, Fevurly RD, Greene AK, Landrigan-Ossar M, Paltiel HJ, Trenor CC, Kozakewich HP |title=Fibro-adipose vascular anomaly: clinical-radiologic-pathologic features of a newly delineated disorder of the extremity |journal=J Pediatr Orthop |volume=34 |issue=1 |pages=109–17 |date=January 2014 |pmid=24322574 |doi=10.1097/BPO.0b013e3182a1f0b8 |url=}}</ref>  
* CLAPO [[syndrome]], a [[syndrome]] diagnosed in 6 patients, is an acronym for [[capillary malformation]] of the lower lip, [[lymphatic malformations]] of the [[face]] and [[neck]], asymmetry, and partial or generalized overgrowth. Manifestations may include [[cutaneous]] [[lesions]] on [[head and neck]] and asymmetrical overgrowth.<ref name="pmid29766551">{{cite journal |vauthors=Downey C, López-Gutiérrez JC, Roé-Crespo E, Puig L, Baselga E |title=Lower lip capillary malformation associated with lymphatic malformation without overgrowth: Part of the spectrum of CLAPO syndrome |journal=Pediatr Dermatol |volume=35 |issue=4 |pages=e243–e244 |date=July 2018 |pmid=29766551 |doi=10.1111/pde.13514 |url=}}</ref><ref name="pmid29446767">{{cite journal |vauthors=Rodriguez-Laguna L, Ibañez K, Gordo G, Garcia-Minaur S, Santos-Simarro F, Agra N, Vallespín E, Fernández-Montaño VE, Martín-Arenas R, Del Pozo Á, González-Pecellín H, Mena R, Rueda-Arenas I, Gomez MV, Villaverde C, Bustamante A, Ayuso C, Ruiz-Perez VL, Nevado J, Lapunzina P, Lopez-Gutierrez JC, Martinez-Glez V |title=CLAPO syndrome: identification of somatic activating PIK3CA mutations and delineation of the natural history and phenotype |journal=Genet. Med. |volume=20 |issue=8 |pages=882–889 |date=August 2018 |pmid=29446767 |doi=10.1038/gim.2017.200 |url=}}</ref>
* [[Somatic]] activating [[mutations]] in PIK3CA that encodes phosphatidylinositol 3-kinase (PI3K), an [[enzyme]] functioning in cell growth, proliferation, differentiation, and survival.<ref name="urlwww.issva.org">{{cite web |url=http://www.issva.org/UserFiles/file/ISSVA-Classification-2018.pdf |title=www.issva.org |format= |work= |accessdate=}}</ref>
* Somatic activating PIK3CA [[mutations]] have been found in [[patients]] with CLAPO [[syndrome]]. This [[gene]] encodes [[proteins]] that function in [[cell-signaling]] pathways.<ref name="pmid29766551" /><ref name="pmid29446767" />
* Clinical and [[radiological]] findings are often sufficient to form the [[diagnosis]]. Inconclusive cases my require [[biopsy]]. [[Surgical resection]] is the often the preferred treatment and is more effective than [[sclerotherapy]], the alternative therapy.<ref name="pmid25298836" /><ref name="pmid24322574" />


==See also==
==See also==

Latest revision as of 19:25, 26 October 2018

Vascular malformation
Classification and external resources
MeSH D054079

For information on vascular anomalies, click here

Vascular Malformation

Home

Overview

Classification

Simple Vascular Malformations
Capillary Malformation
Lymphatic Malformation
Venous Malformation
Arteriovenous Malformation
Arteriovenous Fistula
Combined Vascular Malformations
Vascular Malformations of Major Named Vessels
Vascular Malformations associated With other Anomalies

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Hannan Javed, M.D.[2], Anmol Pitliya, M.B.B.S. M.D.[3]


Overview

Vascular malformation is a blood vessel abnormality. There are many types, but the most common is arteriovenous malformation. Clinical behavior and growth cycles vary widely and it may cause clinical and aesthetic problems. International Society for the Study of Vascular Anomalies (ISSVA) has classified vascular malformation into simple malformation, combined malformation, those of major named vessels, and those associated with other anomalies. Simple malformation have been divided further into capillary malformation, venous malformation and lymphatic malformation.

Classification

 
 
 
 
 
 
Vascular malformations
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Simple vascular malformations
 
Combined vascular malformations
 
Vascular malformations of major named vessels
 
Vascular malformations asscoiated with other anomalies
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
CM + VMCapillary-venous malformationCVM
CM + LMCapillary-lymphatic malformationCLM
CM + AVMCapillary-arteriovenous malformationCAVM
LM + VMLymphatic-venous malformationLVM
CM + LM + VMCapillary-lymphatic-venous malformationCLVM
CM + LM + AVMCapillary-lymphatic-arteriovenous malformationCLVM
CM + VM + AVMCapillary-venous-arteriovenous malformationCVAVM
CM + LM + VM + AVMCapillary-lymphatic-venous-arteriovenous malformationCLVAVM
 

(also known as "channel type" or "truncal" vascular malformations)
Affect
• Lymphatics
• Veins
• Arteries
Anomalies of
• Origin
• Course
• Number
• Diameter (aplasia,
hypoplasia, stenosis,
ectasia / aneurysm)
• Valves
• Communication (AVF)
• Persistence (of
embryonal vessel)
 
Klippel-Trenaunay syndromeCM + VM +/-LM + limb overgrowth
Parke's Weber syndromeCM + AVF + limb overgrowth
Servelle-Martorell syndromeLimb VM + bone undergrowth
Sturge-Weber syndromeFacial + leptomeningeal CM + eye anomalies +/-bone and/or soft tissue overgrowth
Maffucci syndromeVM +/-spindle-cell hemangioma + enchondroma
CLOVES syndromeLM + VM + CM +/-AVM+ lipomatous overgrowth
Proteus syndromeCM, VM and/or LM + asymmetrical somatic overgrowth
Bannayan-Riley-Ruvalcaba syndromelower lip CM + face and neck LM + asymmetry and partial/generalized overgrowth
Limb CM + congenital non-progressive limb overgrowth
Macrocephaly-CM (M-CM / MCAP)
Microcephaly-CM (MICCAP)
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Capillary malformations (CM)
 
Lymphatic malformations (LM)
 
Venous malformations (VM)
 
Arteriovenous malformation (AVM)
 
Arteriovenous fistula
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Nevus simplex / salmon patch, “angel kiss”, “stork bite
 
 
Common (cystic) LM
Macrocystic LM
Microcystic LM
Mixed cystic LM
 
 
Common VM
 
 
Sporadic
 
 
Sporadic
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Cutaneous and/or mucosal CM (also known as “port-wine” stain)
Nonsyndromic CM
• CM with CNS and/or ocular anomalies (Sturge-Weber syndrome)
• CM with bone and/or soft tissues overgrowth
Diffuse CM with overgrowth (DCMO)
 
 
Generalized lymphatic anomaly (GLA)
Kaposiform lymphangiomatosis (KLA)
 
 
Familial VM cutaneo-mucosal (VMCM)
 
 
In HHT
 
 
In HHT
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Reticulate CM
• CM of MIC-CAP (microcephaly-capillary malformation)
• CM of MCAP (megalencephaly-capillary malformation-polymicrogyria)
 
 
LM in Gorham-Stout disease
 
 
Blue rubber bleb nevus (Bean) syndrome VM
 
 
In CM-AVM
 
 
In CM-AVM
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
CM of CM-AVM
 
 
Channel type LM
 
 
Glomuvenous malformation (GVM)
 
 
Others
 
 
Others
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Cutis marmorata telangiectatica congenita (CMTC)
 
 
“Acquired” progressive lymphatic anomaly (so called acquired progressive "lymphangioma")
 
 
Cerebral cavernous malformation (CCM)
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Others
 
 
Primary lymphedema
 
 
Familial intraosseous vascular malformation (VMOS)
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Telangiectasia
Hereditary hemorrhagic telangiectasia (HHT)
• Others
 
 
Others
 
 
Verrucous venous malformation (formerly verrucous hemangioma)
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
 
Others
 
 
 
 
 
 
 
 
 

Abbreviations: CM:capillary malformation; VM:venous malformation; CVM:capillary venous malformation; LM:lymphatic malformation; CLM:capillary lymphatic malformation; AVM:arteriovenous malformation; CAVM:capillary arteriovenous malformation; LVM:lymphatic venous malformation; CLVM:capillary lymphatic venous malformation; CVAVM:capillary venous arteriovenous malformation; CLVAVM:capillary lymphatic venous arteriovenous malformation; AVF:arteriovenous fistula; CLOVES:congenital lipomatous overgrowth, vascular malformations, epidermal nevi, skeletal/scoliosis and spinal abnormalities; M-CM:macrocephaly-capillary malformation; MCAP:megalencephaly-capillary malformation-polymicrogyria; MICCAP:microcephaly-capillary malformation; CNS:central nervous system; DCMO:diffuse capillary malformation with overgrowth; CM-AVM:capillary malformation-arteriovenous malformation; CMTC:cutis marmorata telangiectatica congenita; HHT:hereditary hemorrhagic telangiectasia; GLA:generalized lymphatic anomaly; KLA:kaposiform lymphangiomatosis; VMCM:venous malformation cutaneo mucosal; GVM:glomuvenous malformation; CCM:cerebral cavernous malformation.

Adapted from International Society for the Study of Vascular Anomalies[1]

Simple Vascular Malformations

Simple Vascular Malformations are divided into:

  • Capillary malformation
  • Lymphatic malformation
  • Venous malformation
  • Arteriovenous malformation
  • Arteriovenous fistula

Combined Vascular Malformations

Combined vascular malformations*
CM + VM capillary-venous malformation CVM
CM + LM capillary-lymphatic malformation CLM
CM + AVM capillary-arteriovenous malformation CAVM
LM + VM lymphatic-venous malformation LVM
CM + LM + VM capillary-lymphatic-venous malformation CLVM
CM + LM + AVM capillary-lymphatic-arteriovenous malformation CLAVM
CM + VM + AVM capillary-venous-arteriovenous malformation CVAVM
CM + LM + VM + AVM capillary-lymphatic-venous-arteriovenous m. CLVAVM
Adapted from International Society for the Study of Vascular Anomalies[1]

Abbreviations: CM:capillary malformation; VM:venous malformation; CVM:capillary venous malformation; LM:lymphatic malformation; CLM:capillary lymphatic malformation; AVM:arteriovenous malformation; CAVM:capillary arteriovenous malformation; LVM:lymphatic venous malformation; CLVM:capillary lymphatic venous malformation; CVAVM:capillary venous arteriovenous malformation; CLVAVM:capillary lymphatic venous arteriovenous malformation.

Vascular Malformations of Major Named Vessels

Anomalies of major named vessels

(also known as "channel type" or "truncal" vascular malformations)

Affect
  • lymphatics
  • veins
  • arteries

Anomalies of

  • origin
  • course
  • number
  • length
  • diameter (aplasia, hypoplasia, stenosis, ectasia / aneurysm)
  • valves
  • communication (AVF)
  • persistence (of embryonal vessel)
Adapted from International Society for the Study of Vascular Anomalies[1]

Abbreviations: AVF:arteriovenous fistula.

Vascular Malformations associated With other Anomalies

Vascular malformations associated with other anomalies
Klippel-Trenaunay syndrome* CM + VM +/-LM + limb overgrowth
Parkes Weber syndrome CM + AVF + limb overgrowth
Servelle-Martorell syndrome limb VM + bone undergrowth
Sturge-Weber syndrome facial + leptomeningeal CM + eye anomalies

+/-bone and/or soft tissue overgrowth

Limb CM + congenital non-progressive limb overgrowth
Maffucci syndrome VM +/-spindle-cell hemangioma + enchondroma
Macrocephaly-CM (M-CM / MCAP)*
Microcephaly-CM (MICCAP)
CLOVES syndrome* LM + VM + CM +/-AVM+ lipomatous overgrowth
Proteus syndrome CM, VM and/or LM + asymmetrical somatic overgrowth
Bannayan-Riley-Ruvalcaba syndrome lower lip CM + face and neck LM + asymmetry and partial/generalized overgrowth
Adapted from International Society for the Study of Vascular Anomalies[1]

Abbreviations: CM:capillary malformation; VM:venous malformation; LM:lymphatic malformation; AVM:arteriovenous malformation; AVF:arteriovenous fistula; CLOVES:congenital lipomatous overgrowth, vascular malformations, epidermal nevi, skeletal/scoliosis and spinal abnormalities; M-CM:macrocephaly-capillary malformation; MCAP:megalencephaly-capillary malformation-polymicrogyria; MICCAP:microcephaly-capillary malformation.

Klippel-Trenaunay syndrome

For more information on Klippel-Trenaunay syndrome, click here

Parkes Weber syndrome

For more information on Parkes Weber syndrome, click here.

Servelle-Martorell syndrome

Sturge-Weber syndrome

For more information on Sturge-Weber syndrome, click here.

Maffucci syndrome

For more information on Maffucci syndrome, click here.

CLOVES syndrome

Proteus syndrome

For more information about Proteus syndrome, click here.

Bannayan-Riley-Ruvalcaba syndrome

For more information on Bannayan-Riley-Ruvalcaba syndrome, click here.

CLAPO syndrome

See also

References

  1. 1.0 1.1 1.2 1.3 "Classification | International Society for the Study of Vascular Anomalies".
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  24. Sarman ZS, Yuksel N, Sarman H, Bayramgurler D (June 2014). "Proteus syndrome: report of a case with developmental glaucoma". Korean J Ophthalmol. 28 (3): 272–4. doi:10.3341/kjo.2014.28.3.272. PMC 4038735. PMID 24882963.
  25. Lindhurst MJ, Yourick MR, Yu Y, Savage RE, Ferrari D, Biesecker LG (December 2015). "Repression of AKT signaling by ARQ 092 in cells and tissues from patients with Proteus syndrome". Sci Rep. 5: 17162. doi:10.1038/srep17162. PMC 4675973. PMID 26657992.
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  27. 27.0 27.1 27.2 27.3 Gontijo GM, Pinto CA, Rogatto SR, Cunha IW, Aguiar S, Alves CA (2013). "Bannayan-Riley-Ruvalcaba syndrome with deforming lipomatous hamartomas in infant--case report". An Bras Dermatol. 88 (6): 982–5. doi:10.1590/abd1806-4841.20132730. PMC 3900354. PMID 24474112.
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  30. 30.0 30.1 Downey C, López-Gutiérrez JC, Roé-Crespo E, Puig L, Baselga E (July 2018). "Lower lip capillary malformation associated with lymphatic malformation without overgrowth: Part of the spectrum of CLAPO syndrome". Pediatr Dermatol. 35 (4): e243–e244. doi:10.1111/pde.13514. PMID 29766551.
  31. 31.0 31.1 Rodriguez-Laguna L, Ibañez K, Gordo G, Garcia-Minaur S, Santos-Simarro F, Agra N, Vallespín E, Fernández-Montaño VE, Martín-Arenas R, Del Pozo Á, González-Pecellín H, Mena R, Rueda-Arenas I, Gomez MV, Villaverde C, Bustamante A, Ayuso C, Ruiz-Perez VL, Nevado J, Lapunzina P, Lopez-Gutierrez JC, Martinez-Glez V (August 2018). "CLAPO syndrome: identification of somatic activating PIK3CA mutations and delineation of the natural history and phenotype". Genet. Med. 20 (8): 882–889. doi:10.1038/gim.2017.200. PMID 29446767.
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