Kaposi's Sarcoma (KS)

Kaposi's sarcoma (KS) is a connective tissue cancer caused by Human Herpes Virus 8 - now called Kaposi's sarcoma associated herpesvirus (KSHV). The malignant lesion is characterised by neoplastic cells and abnormally growing blood vessels. KS is named after the hungarian dermatologist, Moritz Kaposi who discovered it in 1872. The viral gene sequence has only been recently determined in 1995-1996. KS is different to other neoplasms by virtue of the fact that lesions may begin in more than one place at the same time.¹

Previous to the occurence of HIV KS was very rare - being mostly isolated to elderly men of Mediterranean, Jewish or African descent.² Patients on immunosuppressants following organ transplantation also accounted for a small number of cases.

During the 1980's the increased number of cases of AIDS was associated with an increased incidence of KS. Fortunately, the widespread use of highly active antiretroviral therapy (HAART) has reduced the number of patients who develop KS. However, KS remains the most frequently reported cancer in some African countries due to untreated HIV e.g. Zimbabwe.
Interestingly, KSHV infection alone does not lead to KS and in Africa male patients who are not HIV positive are more frequently affected than females. Furthermore, familial clustering of KSHV infection has been suggested to occur via nonsexual transmission.³

Risk factors for KS¹

• Gender - men are more often affected
• Ethnicity - Caucasian men and those of Mediterranean, Middle Eastern or African origin
• Men who have sex with men
• Immune deficiency - e.g. post transplant or HIV infection.

• Classic KS - rare, progresses slowly over years and tends to affect old men of Mediterranean or Jewish origin
• Endemic or African KS - young adult men who live near the African equator are affected with KS with a normal immune system. Reported to affect up to 9% of Ugandan men. In some, KS can be aggressive with rapid spread and some children can also be affected which is characterised by lymphatic and lymph node involvement with spread to organs and no skin involvement and is highly fatal
• Transplant related or acquired KS - associated with rapid dissemination
• Epidemic KS - occurrence of KS in patients infected with HIV
• Non-epidemic gay-related KS - KS occurring in homosexual men who do not have HIV. Lesions tend to affect arms, legs and genitalia and progress slowly
• Recurrent KS.

• Lesions may be nodular, papular or blotchy; they may be red, purple, brown or black.
• Lesions sit under or on mucous membranes.
• Commonest sites include mouth, nose and throat.
• Usually painless - but may become painful if inflamed or swollen.
• Lesions may also involve internal organs e.g. lungs (leading to dyspnoea), GIT (can cause fatal bleeding) and lymphatics resulting in lymphoedema.
• There may be superimposed bacterial infection.
• The tumour may disseminate in transplant recipients.
• Very rarely lesions at the oesophagus or respiratory tract may lead to obstruction.

• Spindle cells - elongated tumor cells
• Highly vascular - with dense and irregular blood vessels which leak blood in to the tumour causing the red hue
• There may also be surrounding inflammation.

Definitive diagnosis is based on biopsy features with the presence of spindle cells.Detection of the LANA protein from the virus also confirms the diagnosis.⁴

Other assessment

This should include

• Full history - including sexual history
• Full examination - specifically including lymph node examination and looking at the mucous membranes
• CXR should be performed to pick up any lung involvement
• Other investigations will depend on the presentation e.g. endoscopy or bronchoscopy.

No official system but the AIDS clinical trials group system (ACTG) is most often used. Three elements are used:

• T = extent of tumour
• I = status of immune system according to the CD4 count
• S = extent of involvement of organs or systemic illness.

• KS is incurable but can be controlled with palliative treatment.
• Treat any underlying causes e.g. immunodeficiency or immunosuppression if possible
• AIDS associated KS (epidemic KS) in patients started on HAART will lead to a reduction of lesions in almost 40% of patients although there are a few in whom the KS will grow despite antiretrovirals
• If there are only a few lesions then the following can be considered
  • Radiotherapy
  • Cryotherapy / cryosurgery
  • Surgery - risk of KS appearing in wound edges and probably only appropriate for small surface lesions. Electrodessication with curettage can also be used (tumour cut and edges burnt).
• More widespread KS or organ involvement requires systemic therapy e.g. interferon alfa, liposomal anthracyclines, paclitaxel.

The reduced death rate from AIDS since the 1990's has also resulted in a reduced incidence and severity of KS. Prognosis depends on the type of KS, the immune system status, whether KS is disseminated or not and whether this is the first appearance of KS or recurrence.

It is unclear how KSHV is acquired. There is some research suggesting that the presence of antibodies against KSHV increases the risk of transmission to partner and increases the chances of there being organ involvement.