Lymphangiosarcoma: Difference between revisions
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{{SK}} Stewart-Treves syndrome | {{SK}} Stewart-Treves syndrome | ||
==Overview== | ==Overview== | ||
Lymphangiosarcoma was first discovered by Lowenstein, in 1906, following severe posttraumatic lymphedema of arm for 5 years. Lymphangiosarcoma is a rare malignant tumor which occurs in long-standing cases of primary or secondary [[lymphedema]]. It involves either the upper or lower lymphedemateous extremities but is most common in upper extremities | Lymphangiosarcoma was first discovered by Lowenstein, in 1906, following severe posttraumatic [[lymphedema]] of arm for 5 years. Lymphangiosarcoma is a rare malignant tumor which occurs in long-standing cases of primary or secondary [[lymphedema]]. It involves either the upper or lower lymphedemateous extremities but is most common in upper extremities. Lymphangiosarcoma must be differentiated from other diseases that cause swelling of limb. The prevalence of Stewart-Treves syndrome is approximately 400 worldwide. Common risk factors in the development of lymphangiosarcoma are [[Lymphedema|lymphatic blockage]], [[radiotherapy]], [[mastectomy]], cardiovascular diseases, and [[hypertension]].<ref name="pmid19918554">{{cite journal| author=Sepah YJ, Umer M, Qureshi A, Khan S| title=Lymphangiosarcoma of the arm presenting with lymphedema in a woman 16 years after mastectomy: a case report. | journal=Cases J | year= 2009 | volume= 2 | issue= | pages= 6887 | pmid=19918554 | doi=10.4076/1757-1626-2-6887 | pmc=PMC2769324 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19918554 }} </ref>The sarcoma first appears as a bruise mark, a purplish discolorization or a tender skin nodule in the extremity, typically on the anterior surface. Findings on [[biopsy]] and ultrastructural histologic studies include proliferating vascular channels, hyperchromatism, [[pleomorphism]], [[mitoses]], [[pinocytosis]], intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis. [[Amputation]] of the affected limb is the most common approach to the treatment of lymphangiosarcoma. | ||
==Historical Perspective== | ==Historical Perspective== | ||
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*In 1979, the concept of local immunodeficiency was first identified in the pathogenesis of lymphangiosarcoma by Schreiber.<ref name="pmid23838488">{{cite journal| author=McKeown DG, Boland PJ| title=Stewart-Treves syndrome: a case report. | journal=Ann R Coll Surg Engl | year= 2013 | volume= 95 | issue= 5 | pages= e80-2 | pmid=23838488 | doi=10.1308/003588413X13629960046110 | pmc=PMC4165172 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23838488 }} </ref> | *In 1979, the concept of local immunodeficiency was first identified in the pathogenesis of lymphangiosarcoma by Schreiber.<ref name="pmid23838488">{{cite journal| author=McKeown DG, Boland PJ| title=Stewart-Treves syndrome: a case report. | journal=Ann R Coll Surg Engl | year= 2013 | volume= 95 | issue= 5 | pages= e80-2 | pmid=23838488 | doi=10.1308/003588413X13629960046110 | pmc=PMC4165172 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=23838488 }} </ref> | ||
==Pathophysiology== | ==Pathophysiology== | ||
* Lymphangiosarcoma is a rare malignant tumor which occurs in cases of chronic lymphedema. | * Lymphangiosarcoma is a rare malignant tumor which occurs in cases of chronic [[lymphedema]]. | ||
* Lymphedema is an abnormal collection of protein-rich fluid in the interstitium resulting from obstruction of lymphatic drainage. | * Lymphedema is an abnormal collection of protein-rich fluid in the interstitium resulting from obstruction of [[Lymphatic system|lymphatic]] drainage. | ||
* Lymphatic obstruction causes an increase in the protein content of the extravascular tissue, with subsequent retention of water and swelling of the soft tissue. | * Lymphatic obstruction causes an increase in the [[protein]] content of the extravascular tissue, with subsequent retention of water and swelling of the soft tissue. | ||
* The increase in the extravascular protein stimulates proliferation of fibroblasts, organization of the fluid, and the development of a | * The increase in the extravascular protein stimulates proliferation of [[Fibroblast|fibroblasts]], organization of the fluid, and the development of a [[non pitting]] swelling of the affected extremity. | ||
* Lymphangiosarcoma arises from the endothelial cells of lymphatic vessels or blood vessels. | * Lymphangiosarcoma arises from the [[endothelial cells]] of [[Lymphatic system|lymphatic vessels]] or blood vessels. | ||
* | * | ||
* When it occurs following mastectomy it is known as Stewart-Treves Syndrome.<ref>Stewart FW, Treves N. Lymphangiosarcoma in postmastectomy lymphedema: a report of six cases in elephantiasis chirurgica. Cancer 1948;1:64–81.</ref> | * When it occurs following [[mastectomy]] it is known as Stewart-Treves Syndrome.<ref>Stewart FW, Treves N. Lymphangiosarcoma in postmastectomy lymphedema: a report of six cases in elephantiasis chirurgica. Cancer 1948;1:64–81.</ref> | ||
* Schreiber ''et al.'' proposed that local immunodeficiency as a result of lymphedema results in a "immunologically privileged site" in which the sarcoma is able to develop. | * Schreiber ''et al.'' proposed that local [[immunodeficiency]] as a result of [[lymphedema]] results in a "immunologically privileged site" in which the [[sarcoma]] is able to develop. | ||
*On gross pathology, pachydermatous skin, [[edema]], and reddish blue macules or nodules are characteristic findings of lymphangiosarcoma. | *On gross pathology, pachydermatous skin, [[edema]], and reddish blue [[Macule|macules]] or [[Nodule (medicine)|nodules]] are characteristic findings of lymphangiosarcoma. | ||
*Lymphangiosarcoma can be classified into 3 stages. | *Lymphangiosarcoma can be classified into 3 stages. | ||
**Stage 1 (prolonged lymphedema): | **Stage 1 (prolonged [[lymphedema]]): | ||
*** This stage is characterized by extensive edema that causes the degeneration of fat and collagen mainly in the deep part of the dermis. | *** This stage is characterized by extensive [[edema]] that causes the degeneration of [[fat]] and [[collagen]] mainly in the deep part of the [[dermis]]. | ||
*** Lymphatic blockade causes persistent edema resulting in fibrosis in dermis and subdermis. Stage 2 (premalignant angiomatosis): | *** Lymphatic blockade causes persistent edema resulting in [[fibrosis]] in [[dermis]] and subdermis. | ||
** Stage 2 (premalignant [[angiomatosis]]): | |||
*** This stage involves multiple foci of small, proliferating channels in the dermis and subdermis. | *** This stage involves multiple foci of small, proliferating channels in the dermis and subdermis. | ||
*** These vessels are lined by hyperplastic endothelial cells. | *** These vessels are lined by [[Hyperplasia|hyperplastic]] [[Endothelium|endothelial]] cells. | ||
*** Superficial areas can be seen as bruises or vesicles, whereas deeper areas are seen as areas of induration and | *** Superficial areas can be seen as [[Bruise|bruises]] or [[Vesicle|vesicles]], whereas deeper areas are seen as areas of [[induration]] and [[Bleeding|haemorrhage]]. | ||
*** These aggressive tumors develop from areas of premalignant angiomatosis. | ** Stage 3 ([[malignant]] [[angiosarcoma]]): | ||
*** On microscopic histopathological analysis, proliferating vascular channels, [[hyperchromatism]], pleomorphism, [[mitoses]], pinocytosis, intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis. | *** These aggressive [[Tumor|tumors]] develop from areas of premalignant angiomatosis. | ||
*** On microscopic histopathological analysis, proliferating vascular channels, [[hyperchromatism]], pleomorphism, [[mitoses]], [[pinocytosis]], intercellular junctions, [[Cytoplasm|cytoplasmic]] intermediate [[Protein filament|filaments]], Weibel-Palade bodies, and erythrophagocytosis. | |||
==Causes== | ==Causes== | ||
* Lymphangiosarcoma is caused by chronic lymphedema. | * Lymphangiosarcoma is caused by chronic [[lymphedema]]. | ||
* Causes of lymphedema | * Causes of lymphedema | ||
** Primary lymphedema | ** Primary lymphedema | ||
*** Congenital | *** [[Congenital disorder|Congenital]] | ||
*** Precox (adolescence) | *** Precox ([[adolescence]]) | ||
*** Tarda (adulthood) | *** Tarda (adulthood) | ||
** Secondary lymphedema | ** Secondary lymphedema | ||
*** Malignancy | *** [[Cancer|Malignancy]] | ||
*** Recurrent cellulitis | *** Recurrent [[cellulitis]] | ||
*** Connective tissue disease | *** Connective tissue disease | ||
*** Infection (filariasis) | *** [[Infection]] ([[filariasis]]) | ||
*** Contact dermatitis | *** [[Contact dermatitis]] | ||
*** Lymphatic damage (surgery, radiation therapy, burns, etc) | *** Lymphatic damage (surgery, [[Radiation therapy|radiation]] therapy, [[Burn|burns]], etc) | ||
==Differentiating Lymphangiosarcoma from other Diseases== | ==Differentiating Lymphangiosarcoma from other Diseases== | ||
*Lymphangiosarcoma must be differentiated from other diseases that cause swellling of limb such as: | *Lymphangiosarcoma must be differentiated from other diseases that cause swellling of limb such as: | ||
:* | :*[[Angioedema]] due to C1 inhibitor deficiency | ||
:*Angioendotheliomatosis | :*Angioendotheliomatosis | ||
:*Angiolymphoid hyperplasia with eosinophilia | :*[[Angiolymphoid hyperplasia with eosinophilia]] | ||
:*Cutaneous [[melanoma]] | :*Cutaneous [[melanoma]] | ||
:*[[Hereditary angioedema]] | :*[[Hereditary angioedema]] | ||
:*Lymphangiectasia | :*[[Lymphangiectasia]] | ||
:*Lymphangioma | :*[[Lymphangioma]] | ||
:*Lymphocytoma cutis | :*Lymphocytoma cutis | ||
:*Metastatic breast cancer | :*[[Metastasis|Metastatic]] [[breast cancer]] | ||
:*Malignant melanoma | :*[[Melanoma|Malignant melanoma]] | ||
:*Kaposi sarcoma | :*[[Kaposi's sarcoma|Kaposi sarcoma]] | ||
:*Angiosarcoma | :*[[Angiosarcoma]] | ||
==Epidemiology and Demographics== | ==Epidemiology and Demographics== | ||
* There are 400 cases of lymphangiosarcoma reported worldwide. | * There are 400 cases of lymphangiosarcoma reported worldwide. | ||
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*There is no racial predilection for lymphangiosarcoma. | *There is no racial predilection for lymphangiosarcoma. | ||
==Risk Factors== | ==Risk Factors== | ||
Common risk factors in the development of lymphangiosarcoma are: | |||
* Lymphatic blockage | * [[Lymphatic blockage]] | ||
* Radiotherapy | * [[Radiation therapy|Radiotherapy]] | ||
* Mastectomy | * [[Mastectomy]] | ||
* Cardiovascular diseases | * [[Cardiovascular disease|Cardiovascular diseases]] | ||
* Hypertension.<ref name="pmid19918554">{{cite journal| author=Sepah YJ, Umer M, Qureshi A, Khan S| title=Lymphangiosarcoma of the arm presenting with lymphedema in a woman 16 years after mastectomy: a case report. | journal=Cases J | year= 2009 | volume= 2 | issue= | pages= 6887 | pmid=19918554 | doi=10.4076/1757-1626-2-6887 | pmc=PMC2769324 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19918554 }} </ref> | * [[Hypertension]].<ref name="pmid19918554">{{cite journal| author=Sepah YJ, Umer M, Qureshi A, Khan S| title=Lymphangiosarcoma of the arm presenting with lymphedema in a woman 16 years after mastectomy: a case report. | journal=Cases J | year= 2009 | volume= 2 | issue= | pages= 6887 | pmid=19918554 | doi=10.4076/1757-1626-2-6887 | pmc=PMC2769324 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19918554 }} </ref> | ||
== Natural History, Complications and Prognosis== | == Natural History, Complications and Prognosis== | ||
* History of chronic lymphedema, after mastectomy for breast cancer. | * History of chronic [[lymphedema]], after [[mastectomy]] for [[breast cancer]]. | ||
* Severe chronic edema of an upper extremity usually occurs in patients. | * Severe chronic [[edema]] of an upper extremity usually occurs in patients. | ||
* The skin becomes atrophic and pachydermatous with | * The skin becomes [[Atrophy|atrophic]] and pachydermatous with [[Telangactesia|telangiactesias.]] | ||
* In the area of edema, a puprle patch appears that becomes a subcutaneous nodule, sometimes associated with bleeding and oozing. | * In the area of [[edema]], a puprle patch appears that becomes a subcutaneous [[Nodule (medicine)|nodule]], sometimes associated with [[bleeding]] and oozing. | ||
* With time multiple bluish-reddish nodules appear with ulcer formation, surrounded by areas of necrosis. | * With time multiple bluish-reddish nodules appear with [[ulcer]] formation, surrounded by areas of [[necrosis]]. | ||
* Metastasis appears quickly after nodules are formed, the most common site being the lungs. | * [[Metastasis]] appears quickly after nodules are formed, the most common site being the [[Lung|lungs]]. | ||
* Complications include erysipelas and deep venous | * Complications include [[erysipelas]] and [[Deep vein thrombosis|deep venous thrombosis]] in areas of chronic [[lymphedema]]. | ||
* Other complications include recurrent infections and malignancies. | * Other complications include recurrent [[Infection|infections]] and [[Cancer|malignancies]]. | ||
*Prognosis is generally poor, and the 5 year survival rate of patients with lymphangiosarcoma is approximately less than 5%. | *Prognosis is generally poor, and the 5 year survival rate of patients with lymphangiosarcoma is approximately less than 5%. | ||
== Diagnosis == | == Diagnosis == | ||
=== Symptoms === | === Symptoms === | ||
Symptoms of lymphangiosarcoma | Symptoms of lymphangiosarcoma may include the following: | ||
*Chronic swelling of the affected area. | *Chronic [[Edema|swelling]] of the affected area. | ||
*Painful nodules in the area of swelling. | *Painful [[Nodule (medicine)|nodules]] in the area of swelling. | ||
*Non healing painful ulcers. | *Non healing painful [[Ulcer|ulcers]]. | ||
*Bleeding and oozing from the ulcers. | *[[Bleeding]] and oozing from the ulcers. | ||
=== Physical Examination === | === Physical Examination === | ||
Physical examination may be remarkable for: | Physical examination may be remarkable for: | ||
*Lymphedema- Nontender and non pitting edema of the affected area. | *Lymphedema- Nontender and non pitting [[edema]] of the affected area. | ||
*Lymphangiosarcoma- | *Lymphangiosarcoma- | ||
**Bruise mark. | **[[Bruise]] mark. | ||
**A purplish discolorization. | **A purplish discolorization. | ||
**Tender skin nodule in the extremity, typically on the anterior surface | **Tender skin nodule in the extremity, typically on the anterior surface | ||
** | **[[Ulcecur|Ulce]]<nowiki/>r with crusting. | ||
**Extensive necrosis involving the skin and subcutaneous tissue. | **Extensive [[necrosis]] involving the skin and subcutaneous tissue. | ||
=== Laboratory Findings === | === Laboratory Findings === | ||
*Positive staining for laminin, CD31, collagen IV, and vimentin are specific for angiosarcoma. | *Positive staining for [[Laminin, alpha 1|laminin,]] [[CD31]], [[Collagen, type IV, alpha 1|collagen IV,]] and [[vimentin]] are specific for [[angiosarcoma]]. | ||
===Imaging Findings=== | ===Imaging Findings=== | ||
*[[MRI]] with intravenous contrast is the imaging modality of choice to asses the local extend of lymphangiosarcoma. | *[[MRI]] with intravenous contrast is the imaging modality of choice to asses the local extend of lymphangiosarcoma. | ||
*On [[MRI]], lymphangiosarcoma is characterized by a soft tissue mass with extension through the sub cutaneous tissue and up to the muscle layer with enhancement. | *On [[MRI]], lymphangiosarcoma is characterized by a [[soft tissue]] mass with extension through the sub cutaneous tissue and up to the muscle layer with enhancement. | ||
*Chest radiography and chest CT scan may demonstrate pulmonary metastasis. | *Chest radiography and chest CT scan may demonstrate [[Lung|pulmonary]] [[metastasis]]. | ||
=== Other Diagnostic Studies === | === Other Diagnostic Studies === | ||
*Lymphangiosarcoma may also be diagnosed by measuring antibodies against factor | *Lymphangiosarcoma may also be diagnosed by measuring [[antibodies]] against [[factor VIII]]–related antigen, [[CD34]] antigen, antikeratin antibodies, and positive staining for laminin, CD31, collagen IV, and vimentin. | ||
*Findings on biopsy and ultrastructural histologic studies include proliferating vascular channels, hyperchromatism, pleomorphism, mitoses, pinocytosis, intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis. | *Findings on biopsy and ultrastructural histologic studies include proliferating vascular channels, hyperchromatism, [[pleomorphism]], [[mitoses]], [[pinocytosis]], intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis. | ||
== Treatment == | == Treatment == | ||
=== Medical Therapy === | === Medical Therapy === | ||
*The medical therapy of lymphangiosarcoma is [[paclitaxel]], [[doxorubicin]], [[ifosfamide]], and [[gemcitabine]]. | *The medical therapy of lymphangiosarcoma is [[paclitaxel]], [[doxorubicin]], [[ifosfamide]], and [[gemcitabine]]. | ||
*Treatment of [[lymphedema]] will prevent the development of lymphangiosarcoma. | |||
=== Surgery === | === Surgery === | ||
*Amputation of the affected limb | *[[Amputation]] of the affected limb is the most common approach to the treatment of lymphangiosarcoma. | ||
=== Prevention === | === Prevention === | ||
* | *Treatment of lymphedema is the primary preventive measure available for lymphangiosarcoma. | ||
==References== | ==References== | ||
{{Reflist|2}} | {{Reflist|2}} |
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Ammu Susheela, M.D. [2]
Synonyms and keywords: Stewart-Treves syndrome
Overview
Lymphangiosarcoma was first discovered by Lowenstein, in 1906, following severe posttraumatic lymphedema of arm for 5 years. Lymphangiosarcoma is a rare malignant tumor which occurs in long-standing cases of primary or secondary lymphedema. It involves either the upper or lower lymphedemateous extremities but is most common in upper extremities. Lymphangiosarcoma must be differentiated from other diseases that cause swelling of limb. The prevalence of Stewart-Treves syndrome is approximately 400 worldwide. Common risk factors in the development of lymphangiosarcoma are lymphatic blockage, radiotherapy, mastectomy, cardiovascular diseases, and hypertension.[1]The sarcoma first appears as a bruise mark, a purplish discolorization or a tender skin nodule in the extremity, typically on the anterior surface. Findings on biopsy and ultrastructural histologic studies include proliferating vascular channels, hyperchromatism, pleomorphism, mitoses, pinocytosis, intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis. Amputation of the affected limb is the most common approach to the treatment of lymphangiosarcoma.
Historical Perspective
- Lymphangiosarcoma was first discovered by Lowenstein, in 1906, following severe posttraumatic lymphedema of arm for 5 years
- In 1948, postmastectomy lymphedema was first identified in the pathogenesis of lymphangiosarcoma by Fred Stewart and Norman Treves.
- In 1960, the first homograft skin transplantation was developed to treat lymphangiosarcoma.
- In 1979, the concept of local immunodeficiency was first identified in the pathogenesis of lymphangiosarcoma by Schreiber.[2]
Pathophysiology
- Lymphangiosarcoma is a rare malignant tumor which occurs in cases of chronic lymphedema.
- Lymphedema is an abnormal collection of protein-rich fluid in the interstitium resulting from obstruction of lymphatic drainage.
- Lymphatic obstruction causes an increase in the protein content of the extravascular tissue, with subsequent retention of water and swelling of the soft tissue.
- The increase in the extravascular protein stimulates proliferation of fibroblasts, organization of the fluid, and the development of a non pitting swelling of the affected extremity.
- Lymphangiosarcoma arises from the endothelial cells of lymphatic vessels or blood vessels.
- When it occurs following mastectomy it is known as Stewart-Treves Syndrome.[3]
- Schreiber et al. proposed that local immunodeficiency as a result of lymphedema results in a "immunologically privileged site" in which the sarcoma is able to develop.
- On gross pathology, pachydermatous skin, edema, and reddish blue macules or nodules are characteristic findings of lymphangiosarcoma.
- Lymphangiosarcoma can be classified into 3 stages.
- Stage 1 (prolonged lymphedema):
- Stage 2 (premalignant angiomatosis):
- This stage involves multiple foci of small, proliferating channels in the dermis and subdermis.
- These vessels are lined by hyperplastic endothelial cells.
- Superficial areas can be seen as bruises or vesicles, whereas deeper areas are seen as areas of induration and haemorrhage.
- Stage 3 (malignant angiosarcoma):
- These aggressive tumors develop from areas of premalignant angiomatosis.
- On microscopic histopathological analysis, proliferating vascular channels, hyperchromatism, pleomorphism, mitoses, pinocytosis, intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis.
Causes
- Lymphangiosarcoma is caused by chronic lymphedema.
- Causes of lymphedema
- Primary lymphedema
- Congenital
- Precox (adolescence)
- Tarda (adulthood)
- Secondary lymphedema
- Malignancy
- Recurrent cellulitis
- Connective tissue disease
- Infection (filariasis)
- Contact dermatitis
- Lymphatic damage (surgery, radiation therapy, burns, etc)
- Primary lymphedema
Differentiating Lymphangiosarcoma from other Diseases
- Lymphangiosarcoma must be differentiated from other diseases that cause swellling of limb such as:
- Angioedema due to C1 inhibitor deficiency
- Angioendotheliomatosis
- Angiolymphoid hyperplasia with eosinophilia
- Cutaneous melanoma
- Hereditary angioedema
- Lymphangiectasia
- Lymphangioma
- Lymphocytoma cutis
- Metastatic breast cancer
- Malignant melanoma
- Kaposi sarcoma
- Angiosarcoma
Epidemiology and Demographics
- There are 400 cases of lymphangiosarcoma reported worldwide.
Age
- Lymphangiosarcoma is more commonly observed among middle-aged or elderly.
Gender
- Female are more commonly affected with lymphangiosarcoma than male.
Race
- There is no racial predilection for lymphangiosarcoma.
Risk Factors
Common risk factors in the development of lymphangiosarcoma are:
Natural History, Complications and Prognosis
- History of chronic lymphedema, after mastectomy for breast cancer.
- Severe chronic edema of an upper extremity usually occurs in patients.
- The skin becomes atrophic and pachydermatous with telangiactesias.
- In the area of edema, a puprle patch appears that becomes a subcutaneous nodule, sometimes associated with bleeding and oozing.
- With time multiple bluish-reddish nodules appear with ulcer formation, surrounded by areas of necrosis.
- Metastasis appears quickly after nodules are formed, the most common site being the lungs.
- Complications include erysipelas and deep venous thrombosis in areas of chronic lymphedema.
- Other complications include recurrent infections and malignancies.
- Prognosis is generally poor, and the 5 year survival rate of patients with lymphangiosarcoma is approximately less than 5%.
Diagnosis
Symptoms
Symptoms of lymphangiosarcoma may include the following:
- Chronic swelling of the affected area.
- Painful nodules in the area of swelling.
- Non healing painful ulcers.
- Bleeding and oozing from the ulcers.
Physical Examination
Physical examination may be remarkable for:
- Lymphedema- Nontender and non pitting edema of the affected area.
- Lymphangiosarcoma-
Laboratory Findings
- Positive staining for laminin, CD31, collagen IV, and vimentin are specific for angiosarcoma.
Imaging Findings
- MRI with intravenous contrast is the imaging modality of choice to asses the local extend of lymphangiosarcoma.
- On MRI, lymphangiosarcoma is characterized by a soft tissue mass with extension through the sub cutaneous tissue and up to the muscle layer with enhancement.
- Chest radiography and chest CT scan may demonstrate pulmonary metastasis.
Other Diagnostic Studies
- Lymphangiosarcoma may also be diagnosed by measuring antibodies against factor VIII–related antigen, CD34 antigen, antikeratin antibodies, and positive staining for laminin, CD31, collagen IV, and vimentin.
- Findings on biopsy and ultrastructural histologic studies include proliferating vascular channels, hyperchromatism, pleomorphism, mitoses, pinocytosis, intercellular junctions, cytoplasmic intermediate filaments, Weibel-Palade bodies, and erythrophagocytosis.
Treatment
Medical Therapy
- The medical therapy of lymphangiosarcoma is paclitaxel, doxorubicin, ifosfamide, and gemcitabine.
- Treatment of lymphedema will prevent the development of lymphangiosarcoma.
Surgery
- Amputation of the affected limb is the most common approach to the treatment of lymphangiosarcoma.
Prevention
- Treatment of lymphedema is the primary preventive measure available for lymphangiosarcoma.
References
- ↑ 1.0 1.1 Sepah YJ, Umer M, Qureshi A, Khan S (2009). "Lymphangiosarcoma of the arm presenting with lymphedema in a woman 16 years after mastectomy: a case report". Cases J. 2: 6887. doi:10.4076/1757-1626-2-6887. PMC 2769324. PMID 19918554.
- ↑ McKeown DG, Boland PJ (2013). "Stewart-Treves syndrome: a case report". Ann R Coll Surg Engl. 95 (5): e80–2. doi:10.1308/003588413X13629960046110. PMC 4165172. PMID 23838488.
- ↑ Stewart FW, Treves N. Lymphangiosarcoma in postmastectomy lymphedema: a report of six cases in elephantiasis chirurgica. Cancer 1948;1:64–81.