Kaposi sarcoma: Difference between revisions

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== Further Reading ==
 
== Further Reading ==
   
* Guidelines for the Prevention and Treatment of Opportunistic Infections in Adults and Adolescents with HIV. NIH, CDC, HIVMA, and IDSA. Available at https://clinicalinfo.hiv.gov/en/guidelines/adult-and-adolescent-opportunistic-infection
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* Human Herpesvirus-8 Disease. In: ''Guidelines for the Prevention and Treatment of Opportunistic Infections in Adults and Adolescents with HIV''. NIH, CDC, HIVMA, and IDSA. Available at [https://clinicalinfo.hiv.gov/en/guidelines/hiv-clinical-guidelines-adult-and-adolescent-opportunistic-infections/human-herpesvirus]
   
 
[[Category:Oncology]]
 
[[Category:Oncology]]

Revision as of 07:56, 11 November 2022

Background

  • A tumour associated with HHV-8
  • Closely associated with advanced HIV, but may also present as classic, endemic, or transplant-related KS

ACTG Staging

  • Based on extent of tumour (T), immune status (I), and severity of systemic illness (S)
Criterion Lower Risk (0) Higher risk (1)
Tumour (T) Confined to skin and/or lymph nodes and/or minimal oral disease (non-nodular KS confined to palate) Tumor-associated edema or ulceration; extensive oral KS; gastrointestinal KS; or KS in other non-nodal viscera
Immune status (I) CD4 cell count >200/µL CD4 cell count <200/µL
Systemic illness (S) No history of OI or thrush; no "B" symptoms; and Karnofsky performance status >70 History of OI or thrush; "B" symptoms present; Karnofsky performance status <70; or other HIV-related illness (eg, neurologic disease, lymphoma)
  • However, staging only distinguishes between good risk (T0I0S0) and poor risk (literally all others), used for predicting mortality in the pre-ART era
    • The 3-year survival rate of patients post-ART with T1S1 is about 50%, whereas for T0S0, T1S0, and T0S1 was all 80-90%; immune status does not appear to be predictive[1]

Clinical Manifestations

  • Non-tender, hyperpigmented skin lesions
  • May be macular or nodular
  • Oral lesions in about a third
  • May involve lymphatics, causing severe edema
  • May involve the viscera, which may be asymptomatic or cause dyspnea (lungs), hematochezia or melena (GI tract), or other signs and symptoms
  • Treatment may cause IRIS, either associated with new lesions or with worsening of existing lesions

Management

  • Treatment goals are symptom alleviation, prevention of disease progression, and shrinkage of tumour to alleviate edema, organ compromise, and psychological stress

HIV Patients

Transplant Patients

  • Try to include mTOR inhibitors, such as rapamycin and sirolimus, in the immunosuppression regimens

Local Treatments

  • Intralesional vinblastine 0.2 to 0.3 mg/mL solution with a volume of 0.1 mL per 0.5 cm2 of lesion
    • May be repeated at 3 to 4 weeks
  • Radiation therapy
  • Topical alitretinoin

Systemic Chemotherapy

  • Used in cases of advanced or rapidly-progressive disease
  • Indications include:
    • Symptomatic visceral involvement
    • Widespread skin involvement (eg, more than 25 lesions)
    • Extensive cutaneous KS that is unresponsive to local treatment
    • Extensive edema
    • Immune reconstitution inflammatory syndrome
    • Progression of KS on ART alone

Direct Antivirals

Further Reading

  • Human Herpesvirus-8 Disease. In: Guidelines for the Prevention and Treatment of Opportunistic Infections in Adults and Adolescents with HIV. NIH, CDC, HIVMA, and IDSA. Available at [1]
  1. Nasti G, Talamini R, Antinori A, Martellotta F, Jacchetti G, Chiodo F, Ballardini G, Stoppini L, Di Perri G, Mena M, Tavio M, Vaccher E, D'Arminio Monforte A, Tirelli U; AIDS Clinical Trial Group Staging System in the Haart Era--the Italian Cooperative Group on AIDS and Tumors and the Italian Cohort of Patients Naive from Antiretrovirals. AIDS-related Kaposi's Sarcoma: evaluation of potential new prognostic factors and assessment of the AIDS Clinical Trial Group Staging System in the Haart Era--the Italian Cooperative Group on AIDS and Tumors and the Italian Cohort of Patients Naive From Antiretrovirals. J Clin Oncol. 2003 Aug 1;21(15):2876-82. doi: 10.1200/JCO.2003.10.162. PMID: 12885804.