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Kaposi's sarcoma

Kaposi's sarcoma (KS) is a type of cancer that can form masses on the skin, in lymph nodes, in the mouth, or in other organs.[4][6] The skin lesions are usually painless, purple and may be flat or raised.[6][8] Lesions can occur singly, multiply in a limited area, or may be widespread.[6] Depending on the sub-type of disease and level of immune suppression, KS may worsen either gradually or quickly.[6] Except for Classical KS where there is generally no immune suppression, KS is caused by a combination of immune suppression (such as due to HIV/AIDS) and infection by Human herpesvirus 8 (HHV8 – also called KS-associated herpesvirus (KSHV)).[8]

Kaposi's sarcoma, multiple haemorrhagic sarcoma
Other namesKaposi sarcoma
Kaposi sarcoma. Characteristic purple lesions on the nose of an HIV-positive female.[1]
Pronunciation
SpecialtyOncology
SymptomsPurple colored skin lesions[4]
TypesClassic, endemic, immunosuppression therapy-related, epidemic[4][5]
Risk factorsHuman herpesvirus 8 (HHV8), poor immune function[4][6]
Diagnostic methodTissue biopsy, medical imaging[4][6]
Differential diagnosisBlue rubber bleb nevus syndrome, pyogenic granuloma, melanocytic nevi, melanoma[6]
TreatmentSurgery, chemotherapy, radiation therapy, biologic therapy[4]
Frequency42,000 (new cases, 2018)[7]
Deaths20,000 (2018)[7]

Classic, endemic, immunosuppression therapy-related (also known as iatrogenic), and epidemic (also known as AIDS-related) sub-types are all described.[8] Classic KS tends to affect older men in regions where KSHV is highly prevalent (Mediterranean, Eastern Europe, Middle East), is usually slow-growing, and most often affects only the legs.[8] Endemic KS is most common in Sub-Saharan Africa and is more aggressive in children, while older adults present similarly to classic KS.[8] Immunosuppression therapy-related KS generally occurs in people following organ transplantation and mostly affects the skin.[8] Epidemic KS occurs in people with AIDS and many parts of the body can be affected.[8] KS is diagnosed by tissue biopsy, while the extent of disease may be determined by medical imaging.[4][6][8]

Treatment is based on the sub-type, whether the condition is localized or widespread, and the person's immune function.[6] Localized skin lesions may be treated by surgery, injections of chemotherapy into the lesion, or radiation therapy.[6] Widespread disease may be treated with chemotherapy or biologic therapy.[4][6] In those with HIV/AIDS, highly active antiretroviral therapy (HAART) prevents and often treats KS.[8][9] In certain cases the addition of chemotherapy may be required.[9] With widespread disease, death may occur.[6]

The condition is relatively common in people with HIV/AIDS and following organ transplant.[6][8][9] Over 35% of people with AIDS may be affected.[10] KS was first described by Moritz Kaposi in 1872.[11][12] It became more widely known as one of the AIDS-defining illnesses in the 1980s.[11] KSHV was discovered as a causative agent in 1994.[11][13]

Signs and symptoms edit

KS lesions are nodules or blotches that may be red, purple, brown, or black, and are usually papular.[citation needed]

They are typically found on the skin, but spread elsewhere is common, especially the mouth, gastrointestinal tract and respiratory tract. Growth can range from very slow to explosively fast, and is associated with significant mortality and morbidity.[14]

The lesions are painless, but become cosmetically disfiguring or interruptive to organs.[15]

Skin edit

 
An example of Kaposi's sarcoma
 
Patch stage Kaposi's sarcoma. Red to brownish irregularly shaped macules and plaques.[16]

Commonly affected areas include the lower limbs, back, face, mouth, and genitalia. The lesions are usually as described above, but may occasionally be plaque-like (often on the soles of the feet) or even involved in skin breakdown with resulting fungating lesions. Associated swelling may be from either local inflammation or lymphoedema (obstruction of local lymphatic vessels by the lesion). Kaposi's sarcoma skin lesions may be psychologically distressing.[17][18]

Mouth edit

 
An HIV-positive person presenting with a Kaposi's sarcoma lesion with an overlying candidiasis infection in their mouth

The mouth is involved in about 30% of cases, and is the initial site in 15% of AIDS-related KS. In the mouth, the hard palate is most frequently affected, followed by the gums.[19] Lesions in the mouth may be easily damaged by chewing and bleed or develop secondary infection, and even interfere with eating or speaking.[citation needed]

Gastrointestinal tract edit

Involvement can be common in those with transplant-related or AIDS-related KS, and it may occur in the absence of skin involvement. The gastrointestinal lesions may be silent or cause weight loss, pain, nausea/vomiting, diarrhea, bleeding (either vomiting blood or passing it with bowel movements), malabsorption, or intestinal obstruction.[20]

Respiratory tract edit

Involvement of the airway can present with shortness of breath, fever, cough, coughing up blood or chest pain, or as an incidental finding on chest x-ray.[21] The diagnosis is usually confirmed by bronchoscopy, when the lesions are directly seen and often biopsied. Kaposi's sarcoma of the lung has a poor prognosis.[citation needed]

Cause edit

Kaposi's sarcoma-associated herpesvirus (KSHV), also called HHV-8, is present in almost 100% of Kaposi sarcoma lesions, whether HIV-related, classic, endemic, or iatrogenic.[22] KSHV encodes oncogenes, microRNAs and circular RNAs that promote cancer cell proliferation and escape from the immune system.[23]

Transmission edit

In Europe and North America, KSHV is transmitted through saliva. Thus, kissing is a risk factor for transmission. Higher rates of transmission among gay and bisexual men have been attributed to "deep kissing" sexual partners with KSHV.[24] Another alternative theory suggests that use of saliva as a sexual lubricant might be a major mode for transmission. Prudent advice is to use commercial lubricants when needed and avoid deep kissing with partners with KSHV infection or whose status is unknown.[citation needed]

KSHV is also transmissible via organ transplantation[25] and blood transfusion.[26] Testing for the virus before these procedures is likely to effectively limit iatrogenic transmission.[citation needed]

Pathology edit

 
Micrograph of a Kaposi sarcoma showing its typical features.

Despite its name, in general it is not considered a true sarcoma,[27][28] which is a tumor arising from mesenchymal tissue. The histogenesis of KS remains controversial.[29] KS may arise as a cancer of lymphatic endothelium[30] and forms vascular channels that fill with blood cells, giving the tumor its characteristic bruise-like appearance. KSHV proteins are uniformly detected in KS cancer cells.[citation needed]

KS lesions contain tumor cells with a characteristic abnormal elongated shape, called spindle cells. The most typical feature of Kaposi sarcoma is the presence of spindle cells forming slits containing red blood cells. Mitotic activity is only moderate and pleomorphism is usually absent.[31] The tumor is highly vascular, containing abnormally dense and irregular blood vessels, which leak red blood cells into the surrounding tissue and give the tumor its dark color. Inflammation around the tumor may produce swelling and pain. Variously sized PAS positive hyaline bodies are often seen in the cytoplasm or sometimes extracellularly.[citation needed]

The spindle cells of Kaposi sarcoma differentiate toward endothelial cells, probably of lymph vessel rather than blood vessel origin.[32] The consistent immunoreactivity for podoplanin supports the lymphatic nature of the lesion.[citation needed]

Diagnosis edit

Although KS may be suspected from the appearance of lesions and the patient's risk factors, a definite diagnosis can be made only by biopsy and microscopic examination. Detection of the KSHV protein LANA in tumor cells confirms the diagnosis.[citation needed]

In differential diagnosis, arteriovenous malformations, pyogenic granuloma and other vascular proliferations can be microscopically confused with KS.[33]

Differential diagnosis of Kaposi's sarcoma edit

Source:[34]

  1. Naevus
  2. Histiocytoma
  3. Cryptococcosis
  4. Histoplasmosis
  5. Leishmaniasis
  6. Pneumocystis lesions
  7. Dermatophytosis
  8. Angioma
  9. Bacillary angiomatosis
  10. Pyogenic granuloma
  11. Melanoma

Classification edit

HHV-8 is responsible for all varieties of KS. Since Moritz Kaposi first described the cancer, the disease has been reported in five separate clinical settings, with different presentations, epidemiology, and prognoses.[35]: 599  All of the forms are infected with KSHV and are different manifestations of the same disease but have differences in clinical aggressiveness, prognosis, and treatment.

  • Classic Kaposi sarcoma most commonly appears early on the toes and soles as reddish, violaceous, or bluish-black macules and patches that spread and coalesce to form nodules or plaques.[35]: 599  A small percentage of these patients may have visceral lesions. In most cases the treatment involves surgical removal of the lesion. The condition tends to be indolent and chronic, affecting elderly men from the Mediterranean region, Arab countries,[36] or of Eastern European descent. Israeli Jews have a higher rate of KSHV/HHV-8 infection than European peoples.[37][38]
  • Endemic KS, which has two types. Although this may be present worldwide, it has been originally described later in young African peoples, mainly those from sub-Saharan Africa. This variant is not related to HIV infection[39][40] and is a more aggressive disease that infiltrates the skin extensively.[39][41]
    • African lymphadenopathic Kaposi sarcoma is aggressive, occurring in children under 10 years of age, presenting with lymph node involvement, with or without skin lesions.[35]: 599 
    • African cutaneous Kaposi sarcoma presents with nodular, infiltrative, vascular masses on the extremities, mostly in men between the ages of 20 and 50, and is endemic in tropical Africa.[35]: 599 
  • Immunosuppression-associated Kaposi sarcoma had been described, but only rarely until the advent of calcineurin inhibitors (such as ciclosporines, which are inhibitors of T-cell function) for transplant patients in the 1980s, when its incidence grew rapidly. The tumor arises either when an HHV 8-infected organ is transplanted into someone who has not been exposed to the virus or when the transplant recipient already harbors pre-existing HHV 8 infection.[42][43] Unlike classic Kaposi sarcoma, the site of presentation is more variable.[35]: 600 
  • AIDS-associated Kaposi sarcoma typically presents with cutaneous lesions that begin as one or several red to purple-red macules, rapidly progressing to papules, nodules, and plaques, with a predilection for the head, back, neck, trunk, and mucous membranes. In more advanced cases, lesions can be found in the stomach and intestines, the lymph nodes, and the lungs.[35]: 599  Compared to other forms of KS, KS-AIDS stimulated more interest in KS research, as it was one of the first illnesses associated with AIDS and first described in 1981.[44][45][46] This form of KS is over 300 times more common in AIDS patients than in renal transplant recipients. In this case, HHV 8 is sexually transmitted among people also at risk for sexually transmitted HIV infection.[47]

Prevention edit

Blood tests to detect antibodies against KSHV have been developed and can be used to determine whether a person is at risk for transmitting the infection to their sexual partner, or whether an organ is infected before transplantation. However, these tests are not available except as research tools, and, thus, there is little screening for persons at risk for becoming infected with KSHV, such as people following a transplant.[citation needed]

Treatment edit

Kaposi sarcoma is not curable, but it can often be treatable for many years. In KS associated with immunodeficiency or immunosuppression, treating the cause of the immune system dysfunction can slow or stop the progression of KS. In 40% or more of patients with AIDS-associated Kaposi sarcoma, the Kaposi lesions will shrink upon first starting highly active antiretroviral therapy (HAART). Therefore, HAART is considered the cornerstone of therapy in AIDS-associated Kaposi sarcoma. However, in a certain percentage[vague] of such people, Kaposi sarcoma may recur after many years on HAART, especially if HIV is not completely suppressed.

People with a few local lesions can often be treated with local measures such as radiation therapy or cryosurgery.[48][49] Weak evidence suggests that antiretroviral therapy in combination with chemotherapy is more effective than either of those two therapies individually.[50] Limited basic and clinical evidence suggest that topical beta-blockers, such as timolol, may induce regression of localized lesions in classic as well as HIV-associated Kaposi sarcoma.[51][52] In general, surgery is not recommended, as Kaposi sarcoma can appear in wound edges. In general, more widespread disease, or disease affecting internal organs, is treated with systemic therapy with interferon alpha, liposomal anthracyclines (such as liposomal doxorubicin or daunorubicin), thalidomide, or paclitaxel.[53][54]

Alitretinoin, applied to the lesion, may be used when the lesion is not getting better with standard treatment of HIV/AIDS and chemotherapy or radiation therapy cannot be used.[55]

Epidemiology edit

With the decrease in the death rate among people with HIV/AIDS receiving new treatments in the 1990s, the rates and severity of epidemic KS also decreased. However, the number of people living with HIV/AIDS is increasing in the United States, and it is possible that the number of people with AIDS-associated Kaposi sarcoma will again rise as these people live longer with HIV infection.[citation needed]

Society edit

Because of their highly visible nature, external lesions are sometimes the presenting symptom of AIDS. Kaposi sarcoma entered the awareness of the general public with the release of the film Philadelphia, in which the main character was fired after his employers found out he was HIV-positive due to visible lesions. By the time KS lesions appear, likely, the immune system has already been severely weakened.[citation needed] It has been reported that only 6% of men who have sex with men are aware that KS is caused by a virus different from HIV.[56] Thus, there is little community effort to prevent KSHV infection. Likewise, no systematic screening of organ donations is in place.

In people with AIDS, Kaposi sarcoma is considered an opportunistic infection, a disease that can gain a foothold in the body because the immune system has been weakened. With the rise of HIV/AIDS in Africa, where KSHV is widespread, KS has become the most frequently reported cancer in some countries.

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External links edit

kaposi, sarcoma, type, cancer, that, form, masses, skin, lymph, nodes, mouth, other, organs, skin, lesions, usually, painless, purple, flat, raised, lesions, occur, singly, multiply, limited, area, widespread, depending, type, disease, level, immune, suppressi. Kaposi s sarcoma KS is a type of cancer that can form masses on the skin in lymph nodes in the mouth or in other organs 4 6 The skin lesions are usually painless purple and may be flat or raised 6 8 Lesions can occur singly multiply in a limited area or may be widespread 6 Depending on the sub type of disease and level of immune suppression KS may worsen either gradually or quickly 6 Except for Classical KS where there is generally no immune suppression KS is caused by a combination of immune suppression such as due to HIV AIDS and infection by Human herpesvirus 8 HHV8 also called KS associated herpesvirus KSHV 8 Kaposi s sarcoma multiple haemorrhagic sarcomaOther namesKaposi sarcomaKaposi sarcoma Characteristic purple lesions on the nose of an HIV positive female 1 Pronunciation k ae ˈ p oʊ s i z 2 ˈ k ɑː p e s i z ˈ k ae p e 3 SpecialtyOncologySymptomsPurple colored skin lesions 4 TypesClassic endemic immunosuppression therapy related epidemic 4 5 Risk factorsHuman herpesvirus 8 HHV8 poor immune function 4 6 Diagnostic methodTissue biopsy medical imaging 4 6 Differential diagnosisBlue rubber bleb nevus syndrome pyogenic granuloma melanocytic nevi melanoma 6 TreatmentSurgery chemotherapy radiation therapy biologic therapy 4 Frequency42 000 new cases 2018 7 Deaths20 000 2018 7 Classic endemic immunosuppression therapy related also known as iatrogenic and epidemic also known as AIDS related sub types are all described 8 Classic KS tends to affect older men in regions where KSHV is highly prevalent Mediterranean Eastern Europe Middle East is usually slow growing and most often affects only the legs 8 Endemic KS is most common in Sub Saharan Africa and is more aggressive in children while older adults present similarly to classic KS 8 Immunosuppression therapy related KS generally occurs in people following organ transplantation and mostly affects the skin 8 Epidemic KS occurs in people with AIDS and many parts of the body can be affected 8 KS is diagnosed by tissue biopsy while the extent of disease may be determined by medical imaging 4 6 8 Treatment is based on the sub type whether the condition is localized or widespread and the person s immune function 6 Localized skin lesions may be treated by surgery injections of chemotherapy into the lesion or radiation therapy 6 Widespread disease may be treated with chemotherapy or biologic therapy 4 6 In those with HIV AIDS highly active antiretroviral therapy HAART prevents and often treats KS 8 9 In certain cases the addition of chemotherapy may be required 9 With widespread disease death may occur 6 The condition is relatively common in people with HIV AIDS and following organ transplant 6 8 9 Over 35 of people with AIDS may be affected 10 KS was first described by Moritz Kaposi in 1872 11 12 It became more widely known as one of the AIDS defining illnesses in the 1980s 11 KSHV was discovered as a causative agent in 1994 11 13 Contents 1 Signs and symptoms 1 1 Skin 1 2 Mouth 1 3 Gastrointestinal tract 1 4 Respiratory tract 2 Cause 2 1 Transmission 3 Pathology 4 Diagnosis 4 1 Differential diagnosis of Kaposi s sarcoma 4 2 Classification 5 Prevention 6 Treatment 7 Epidemiology 8 Society 9 References 10 External linksSigns and symptoms editKS lesions are nodules or blotches that may be red purple brown or black and are usually papular citation needed They are typically found on the skin but spread elsewhere is common especially the mouth gastrointestinal tract and respiratory tract Growth can range from very slow to explosively fast and is associated with significant mortality and morbidity 14 The lesions are painless but become cosmetically disfiguring or interruptive to organs 15 Skin edit nbsp An example of Kaposi s sarcoma nbsp Patch stage Kaposi s sarcoma Red to brownish irregularly shaped macules and plaques 16 Commonly affected areas include the lower limbs back face mouth and genitalia The lesions are usually as described above but may occasionally be plaque like often on the soles of the feet or even involved in skin breakdown with resulting fungating lesions Associated swelling may be from either local inflammation or lymphoedema obstruction of local lymphatic vessels by the lesion Kaposi s sarcoma skin lesions may be psychologically distressing 17 18 Mouth edit nbsp An HIV positive person presenting with a Kaposi s sarcoma lesion with an overlying candidiasis infection in their mouth The mouth is involved in about 30 of cases and is the initial site in 15 of AIDS related KS In the mouth the hard palate is most frequently affected followed by the gums 19 Lesions in the mouth may be easily damaged by chewing and bleed or develop secondary infection and even interfere with eating or speaking citation needed Gastrointestinal tract edit Involvement can be common in those with transplant related or AIDS related KS and it may occur in the absence of skin involvement The gastrointestinal lesions may be silent or cause weight loss pain nausea vomiting diarrhea bleeding either vomiting blood or passing it with bowel movements malabsorption or intestinal obstruction 20 Respiratory tract edit Involvement of the airway can present with shortness of breath fever cough coughing up blood or chest pain or as an incidental finding on chest x ray 21 The diagnosis is usually confirmed by bronchoscopy when the lesions are directly seen and often biopsied Kaposi s sarcoma of the lung has a poor prognosis citation needed Cause editKaposi s sarcoma associated herpesvirus KSHV also called HHV 8 is present in almost 100 of Kaposi sarcoma lesions whether HIV related classic endemic or iatrogenic 22 KSHV encodes oncogenes microRNAs and circular RNAs that promote cancer cell proliferation and escape from the immune system 23 Transmission edit In Europe and North America KSHV is transmitted through saliva Thus kissing is a risk factor for transmission Higher rates of transmission among gay and bisexual men have been attributed to deep kissing sexual partners with KSHV 24 Another alternative theory suggests that use of saliva as a sexual lubricant might be a major mode for transmission Prudent advice is to use commercial lubricants when needed and avoid deep kissing with partners with KSHV infection or whose status is unknown citation needed KSHV is also transmissible via organ transplantation 25 and blood transfusion 26 Testing for the virus before these procedures is likely to effectively limit iatrogenic transmission citation needed Pathology edit nbsp Micrograph of a Kaposi sarcoma showing its typical features Despite its name in general it is not considered a true sarcoma 27 28 which is a tumor arising from mesenchymal tissue The histogenesis of KS remains controversial 29 KS may arise as a cancer of lymphatic endothelium 30 and forms vascular channels that fill with blood cells giving the tumor its characteristic bruise like appearance KSHV proteins are uniformly detected in KS cancer cells citation needed KS lesions contain tumor cells with a characteristic abnormal elongated shape called spindle cells The most typical feature of Kaposi sarcoma is the presence of spindle cells forming slits containing red blood cells Mitotic activity is only moderate and pleomorphism is usually absent 31 The tumor is highly vascular containing abnormally dense and irregular blood vessels which leak red blood cells into the surrounding tissue and give the tumor its dark color Inflammation around the tumor may produce swelling and pain Variously sized PAS positive hyaline bodies are often seen in the cytoplasm or sometimes extracellularly citation needed The spindle cells of Kaposi sarcoma differentiate toward endothelial cells probably of lymph vessel rather than blood vessel origin 32 The consistent immunoreactivity for podoplanin supports the lymphatic nature of the lesion citation needed nbsp Micrograph of a Kaposi sarcoma showing the characteristic spindle cells high vascularity and intracellular hyaline globs H amp E stain nbsp Micrograph of promontory sign in Kaposi s sarcoma in patch stage Dilated irregular vascular channels surround a pre existing vessel 16 nbsp Micrograph of plaque stage with bizarre vessels dissecting the upper dermis There is erythrocyte extravasation and hemosiderin pigmentation 16 nbsp Micrograph of tumor stage Well circumscribed spindle cell tumor Erythrocytes lie within poorly defined slit like vascular spaces 16 Diagnosis editAlthough KS may be suspected from the appearance of lesions and the patient s risk factors a definite diagnosis can be made only by biopsy and microscopic examination Detection of the KSHV protein LANA in tumor cells confirms the diagnosis citation needed In differential diagnosis arteriovenous malformations pyogenic granuloma and other vascular proliferations can be microscopically confused with KS 33 Differential diagnosis of Kaposi s sarcoma edit Source 34 Naevus Histiocytoma Cryptococcosis Histoplasmosis Leishmaniasis Pneumocystis lesions Dermatophytosis Angioma Bacillary angiomatosis Pyogenic granuloma Melanoma Classification edit HHV 8 is responsible for all varieties of KS Since Moritz Kaposi first described the cancer the disease has been reported in five separate clinical settings with different presentations epidemiology and prognoses 35 599 All of the forms are infected with KSHV and are different manifestations of the same disease but have differences in clinical aggressiveness prognosis and treatment Classic Kaposi sarcoma most commonly appears early on the toes and soles as reddish violaceous or bluish black macules and patches that spread and coalesce to form nodules or plaques 35 599 A small percentage of these patients may have visceral lesions In most cases the treatment involves surgical removal of the lesion The condition tends to be indolent and chronic affecting elderly men from the Mediterranean region Arab countries 36 or of Eastern European descent Israeli Jews have a higher rate of KSHV HHV 8 infection than European peoples 37 38 Endemic KS which has two types Although this may be present worldwide it has been originally described later in young African peoples mainly those from sub Saharan Africa This variant is not related to HIV infection 39 40 and is a more aggressive disease that infiltrates the skin extensively 39 41 African lymphadenopathic Kaposi sarcoma is aggressive occurring in children under 10 years of age presenting with lymph node involvement with or without skin lesions 35 599 African cutaneous Kaposi sarcoma presents with nodular infiltrative vascular masses on the extremities mostly in men between the ages of 20 and 50 and is endemic in tropical Africa 35 599 Immunosuppression associated Kaposi sarcoma had been described but only rarely until the advent of calcineurin inhibitors such as ciclosporines which are inhibitors of T cell function for transplant patients in the 1980s when its incidence grew rapidly The tumor arises either when an HHV 8 infected organ is transplanted into someone who has not been exposed to the virus or when the transplant recipient already harbors pre existing HHV 8 infection 42 43 Unlike classic Kaposi sarcoma the site of presentation is more variable 35 600 AIDS associated Kaposi sarcoma typically presents with cutaneous lesions that begin as one or several red to purple red macules rapidly progressing to papules nodules and plaques with a predilection for the head back neck trunk and mucous membranes In more advanced cases lesions can be found in the stomach and intestines the lymph nodes and the lungs 35 599 Compared to other forms of KS KS AIDS stimulated more interest in KS research as it was one of the first illnesses associated with AIDS and first described in 1981 44 45 46 This form of KS is over 300 times more common in AIDS patients than in renal transplant recipients In this case HHV 8 is sexually transmitted among people also at risk for sexually transmitted HIV infection 47 Prevention editBlood tests to detect antibodies against KSHV have been developed and can be used to determine whether a person is at risk for transmitting the infection to their sexual partner or whether an organ is infected before transplantation However these tests are not available except as research tools and thus there is little screening for persons at risk for becoming infected with KSHV such as people following a transplant citation needed Treatment editKaposi sarcoma is not curable but it can often be treatable for many years In KS associated with immunodeficiency or immunosuppression treating the cause of the immune system dysfunction can slow or stop the progression of KS In 40 or more of patients with AIDS associated Kaposi sarcoma the Kaposi lesions will shrink upon first starting highly active antiretroviral therapy HAART Therefore HAART is considered the cornerstone of therapy in AIDS associated Kaposi sarcoma However in a certain percentage vague of such people Kaposi sarcoma may recur after many years on HAART especially if HIV is not completely suppressed People with a few local lesions can often be treated with local measures such as radiation therapy or cryosurgery 48 49 Weak evidence suggests that antiretroviral therapy in combination with chemotherapy is more effective than either of those two therapies individually 50 Limited basic and clinical evidence suggest that topical beta blockers such as timolol may induce regression of localized lesions in classic as well as HIV associated Kaposi sarcoma 51 52 In general surgery is not recommended as Kaposi sarcoma can appear in wound edges In general more widespread disease or disease affecting internal organs is treated with systemic therapy with interferon alpha liposomal anthracyclines such as liposomal doxorubicin or daunorubicin thalidomide or paclitaxel 53 54 Alitretinoin applied to the lesion may be used when the lesion is not getting better with standard treatment of HIV AIDS and chemotherapy or radiation therapy cannot be used 55 Epidemiology editWith the decrease in the death rate among people with HIV AIDS receiving new treatments in the 1990s the rates and severity of epidemic KS also decreased However the number of people living with HIV AIDS is increasing in the United States and it is possible that the number of people with AIDS associated Kaposi sarcoma will again rise as these people live longer with HIV infection citation needed Society editThis section needs additional citations for verification Please help improve this article by adding citations to reliable sources in this section Unsourced material may be challenged and removed Find sources Kaposi s sarcoma news newspapers books scholar JSTOR November 2020 Learn how and when to remove this message Because of their highly visible nature external lesions are sometimes the presenting symptom of AIDS Kaposi sarcoma entered the awareness of the general public with the release of the film Philadelphia in which the main character was fired after his employers found out he was HIV positive due to visible lesions By the time KS lesions appear likely the immune system has already been severely weakened citation needed It has been reported that only 6 of men who have sex with men are aware that KS is caused by a virus different from HIV 56 Thus there is little community effort to prevent KSHV infection Likewise no systematic screening of organ donations is in place In people with AIDS Kaposi sarcoma is considered an opportunistic infection a disease that can gain a foothold in the body because the immune system has been weakened With the rise of HIV AIDS in Africa where KSHV is widespread KS has become the most frequently reported cancer in some countries References edit Sand M Sand D Thrandorf C Paech V Altmeyer P Bechara FG June 2010 Cutaneous lesions of the nose Head amp Face Medicine 6 7 doi 10 1186 1746 160X 6 7 PMC 2903548 PMID 20525327 Collins English Dictionary Complete and Unabridged 12th Edition 2014 S v 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1985 Differential diagnosis of Kaposi s sarcoma Archives of Pathology amp Laboratory Medicine 109 2 123 127 PMID 2983633 Griffiths C Barker J Bleiker TO Chalmers R Creamer D 4 April 2016 Rook s textbook of dermatology Ninth ed p 31 29 ISBN 9781118441190 a b c d e f James W Berger T Elston D 2005 Andrews Diseases of the Skin Clinical Dermatology 10th ed Saunders ISBN 978 0 7216 2921 6 Kumar P 2011 Classic Kaposi s sarcoma in Arabs widening ethnic involvement Journal of Cancer Research and Therapeutics 7 1 92 4 doi 10 4103 0973 1482 80456 PMID 21546753 Iscovich J Boffetta P Winkelmann R Brennan P Azizi E October 1998 Classic Kaposi s sarcoma in Jews living in Israel 1961 1989 a population based incidence study AIDS 12 15 2067 72 doi 10 1097 00002030 199815000 00019 PMID 9814876 S2CID 23848900 Fenig E Brenner B Rakowsky E Lapidoth M Katz A Sulkes A October 1998 Classic Kaposi sarcoma experience at Rabin Medical Center in Israel American Journal of Clinical Oncology 21 5 498 500 doi 10 1097 00000421 199810000 00016 PMID 9781608 a b Cook Mozaffari P Newton R Beral V Burkitt DP December 1998 The geographical distribution of Kaposi s sarcoma and of lymphomas in Africa before the AIDS epidemic British Journal of Cancer 78 11 1521 8 doi 10 1038 bjc 1998 717 PMC 2063225 PMID 9836488 Olsen SJ Chang Y Moore PS Biggar RJ Melbye M October 1998 Increasing Kaposi s sarcoma associated herpesvirus seroprevalence with age in a highly Kaposi s sarcoma endemic region Zambia in 1985 AIDS 12 14 1921 5 doi 10 1097 00002030 199814000 00024 PMID 9792393 S2CID 1734745 Olsen SJ Chang Y Moore PS Biggar RJ Melbye M October 1998 Increasing Kaposi s sarcoma associated herpesvirus seroprevalence with age in a highly Kaposi s sarcoma endemic region Zambia in 1985 AIDS 12 14 1921 5 doi 10 1097 00002030 199814000 00024 PMID 9792393 S2CID 1734745 Qunibi W Al Furayh O Almeshari K Lin SF Sun R Heston L Ross D Rigsby M Miller G February 1998 Serologic association of human herpesvirus eight with posttransplant Kaposi s sarcoma in Saudi Arabia Transplantation 65 4 583 5 doi 10 1097 00007890 199802270 00024 PMID 9500639 Luppi M Barozzi P Schulz TF Setti G Staskus K Trovato R Narni F Donelli A Maiorana A Marasca R Sandrini S Torelli G November 2000 Bone marrow failure associated with human herpesvirus 8 infection after transplantation The New England Journal of Medicine 343 19 1378 85 doi 10 1056 NEJM200011093431905 PMID 11070102 Borkovic SP Schwartz RA December 1981 Kaposi s sarcoma presenting in the homosexual man a new and striking phenomenon Arizona Medicine 38 12 902 4 PMID 7332494 Hausen HZ 2006 Rhadinoviruses Infections Causing Human Cancer Weinheim Wiley VCH Drabell FG 2006 Kaposi s Sarcoma and Renal Diseases New Topics in Cancer Research New York Nova Biomedical Books Beral V Peterman TA Berkelman RL Jaffe HW January 1990 Kaposi s sarcoma among persons with AIDS a sexually transmitted infection Lancet 335 8682 123 8 doi 10 1016 0140 6736 90 90001 L PMID 1967430 S2CID 35639169 Tappero JW Berger TG Kaplan LD Volberding PA Kahn JO 1991 Cryotherapy for cutaneous Kaposi s sarcoma KS associated with acquired immune deficiency syndrome AIDS a phase II trial Journal of Acquired Immune Deficiency Syndromes 4 9 839 46 doi 10 1097 00126334 199109000 00002 PMID 1895204 S2CID 19909703 Zimmerman EE Crawford P December 2012 Cutaneous cryosurgery American Family Physician 86 12 1118 24 PMID 23316984 Anglemyer A Agrawal AK Rutherford GW January 2014 Treatment of Kaposi sarcoma in children with HIV 1 infection The Cochrane Database of Systematic Reviews 1 1 CD009826 doi 10 1002 14651858 CD009826 pub2 PMID 24464843 McAllister SC Hanson RS Manion RD November 2015 Propranolol Decreases Proliferation of Endothelial Cells Transformed by Kaposi s Sarcoma Associated Herpesvirus and Induces Lytic Viral Gene Expression Journal of Virology 89 21 11144 9 doi 10 1128 JVI 01569 15 PMC 4621132 PMID 26269192 Abdelmaksoud A Filoni A Giudice G Vestita M January 2017 Classic and HIV related Kaposi sarcoma treated with 0 1 topical timolol gel Journal of the American Academy of Dermatology 76 1 153 155 doi 10 1016 j jaad 2016 08 041 PMID 27986137 Gill PS Tulpule A Espina BM Cabriales S Bresnahan J Ilaw M Louie S Gustafson NF Brown MA Orcutt C Winograd B Scadden DT June 1999 Paclitaxel is safe and effective in the treatment of advanced AIDS related Kaposi s sarcoma Journal of Clinical Oncology 17 6 1876 83 doi 10 1200 jco 1999 17 6 1876 PMID 10561228 Sgadari C Toschi E Palladino C Barillari G Carlei D Cereseto A Ciccolella C Yarchoan R Monini P Sturzl M Ensoli B July 2000 Mechanism of paclitaxel activity in Kaposi s sarcoma Journal of Immunology 165 1 509 17 doi 10 4049 jimmunol 165 1 509 PMID 10861090 Summary of Product Characteristics PDF EMA Retrieved 14 March 2020 Phillips AM Jones AG Osmond DH Pollack LM Catania JA Martin JN December 2008 Awareness of Kaposi s sarcoma associated herpesvirus among men who have sex with men Sexually Transmitted Diseases 35 12 1011 4 doi 10 1097 OLQ 0b013e318182c91f PMC 2593118 PMID 18665016 External links editKaposi sarcoma photo library at Dermnet Archived 2010 11 08 at the Wayback Machine Retrieved from https en wikipedia org w index php title Kaposi 27s sarcoma amp oldid 1220515405, wikipedia, wiki, book, books, library,

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