Furthermore, antiviral treatment, which has led to a clinical improvement, has been shown to reduce HHV8 viral load in patients with KS [63], PEL and haemophagocytic syndrome [64]. In a series of three patients treated with ganciclovir, there was
a reduction in the frequency of acute symptoms of MCD for two patients treated with oral and intravenous ganciclovir [65]. For the third patient, there was resolution of pulmonary and renal failure with intravenous ganciclovir. All the patients had a reduction in HHV8 viral load with the ganciclovir therapy, accompanying the resolution of their symptoms. However, the use of foscarnet and cidofovir antiviral therapy was ineffective in an HIV-negative MCD patient with proven HHV8 viraemia and treatment with corticosteroids in combination with see more chlorambucil
chemotherapy was required to achieve a clinical response [66]. Furthermore, the HHV8 viral load rose in this patient with the commencement of anti-herpesvirus therapy; this may indicate that the antiviral therapy was ineffective in this case, or that, once the MCD is established, HHV8 has a less prominent role and antiviral therapy is less ALK inhibitor effective than immunotherapy or chemotherapy. Casper et al. [36] randomized 26 men with HHV8 infection to receive 8 weeks of valganciclovir administered orally (900 mg once per day) or 8 weeks Forskolin purchase of placebo. After a 2-week washout period, participants in each group received the study drug they had not yet taken (either valganciclovir or placebo), for 8 additional
weeks. Oral swab samples were collected daily during the study, and HHV8 and CMV DNA were quantified by real-time PCR. A total of 16 HIV-positive men and 10 HIV-negative men enrolled in, and completed the study. Of the 3439 swab samples that participants had been expected to provide, 3029 (88%) were available for analysis. HHV8 was detected on 44% of swabs collected from participants who were receiving placebo, compared with 23% of swabs collected from participants who were receiving valganciclovir (relative risk [RR] 0.54, 95% CI: 0.33–0.90; p = 0.02). Valganciclovir reduced oropharyngeal shedding of cytomegalovirus by 80% (RR: 0.20, 95% CI: 0.08–0.48; p < 0.001). Shedding of HHV8 and shedding of cytomegalovirus were independent. Haematological, renal, or hepatic toxicities were no more common among participants who received the active drug, compared with those who received placebo, though participants who received valganciclovir reported more days of diarrhoea. Valganciclovir administered orally once per day is well tolerated and significantly reduces the frequency and quantity of HHV8 replication. A further study [67] compared the efficacy of valaciclovir, famciclovir and cART in reducing HHV8 oropharyngeal shedding in 6036 swabs from 58 participants.