Background: The role of intermittent antiretroviral therapy in chronic HIV infection is still controversial.

Methods: ISS-PART is an ongoing prospective, randomized, multicenter clinical trial of STI in subjects with chronic HIV infection and stable control of viral replication. Subjects are randomized to: 1) Arm A: Standard of care for 24 months (mos), and 2) Arm B : Intermittent antiretroviral treatment (5 STI of 1-, 1-, 2-, 2-, and 3-mos duration, each one followed by 3 mos on therapy). Study endpoint is the proportion of pts with CD4 > 500/mmc at month 24.

Results: A total of 273 (136 in arm B) subjects was enrolled. Mean age 40.1 yrs; sex F (30.3%); NNRTI-including regimens 67.6%; mean HAART duration 26 mos; median CD4 at randomization 691/mmc; median CD4 pre-HAART 393/mmc.

After a median follow up of 6 mos, dropout rate is 3.6% in arm A and 13.2% in arm B. Preliminary observations show the following:

	1^st STI ( 1 mo)	2^nd STI (1 mo)	3^rd STI ( 2 mos)
	134 pts	92 pts	34 pts
Median rebound in HIV-RNA (log)	+2.3	+2.1	+2.2
Subjects with no HIV-RNA rebound	33 (24.6%)	25 (27.2%)	3 (8.8%)
Median decrease in CD4 absolute number	-72	-60	-147
Subjects with > 25% reduction in CD4	26 (19.4%)	15 (16.3%)	7 (20.6%)

At therapy reinitiation, after each STI, median CD4 have returned to baseline values. After the 1^st, 2^nd and 3^rd STI 88.9%, 96.8% and 100% of patients have achieved HIV RNA < 400 copies/ml. Genotypic resistance tests performed during STIs have shown resistance associated mutations in 29 (21.3%) patients of arm B at any time off therapy. All but two achieved viremia levels below 400 copies after the reinitiation of their pre-STI antiretroviral regimen.

Conclusions: Overall response to therapy reinitiation was satisfactory; however, a longer follow-up is required to assess the clinical significance of mutations in the rebounding virus.