32 (0 13, 0 66)/100 PYFU) than FTC-episodes (0 18 (0 10, 0 30)/10

32 (0.13, 0.66)/100 PYFU) than FTC-episodes (0.18 (0.10, 0.30)/100 PYFU). However, in univariable analyses, no significant difference was seen between type of regimen and detection of K65R (RR: 1.77 (95% CI: 0.71, 4.38) comparing 3TC- to FTC- episodes). Sex, age, risk group, year of starting regimen and ethnicity were not significant in univariable analyses and were excluded from multivariable

analyses. After adjusting for current CD4 count and viral load, the association between type of regimen and K65R remained non-significant (1.62 (0.65, 4.02)) (Table 2). Patients with higher current CD4 counts were less likely to develop K65R (0.77 (0.65, 0.91) per 50 cells higher (p = 0.001)), and currently viraemic patients were more likely to develop K65R (5.31 (2.51, 11.24) comparing viral load >50 copies/ml to viral load ≤50 copies/ml). No other factors were significantly associated with www.selleckchem.com/products/BIBF1120.html the detection of K65R ( Table 2). The overall event rate for the detection of M184V was higher than that of K65R. Thirty-eight cases of M184V were detected, giving an event rate of 0.38 (95% CI: 0.26, 0.50)/100 PYFU. M184V development was commoner in 3TC-episodes than FTC-episodes (0.55 (0.28, 0.96) vs. 0.34 (0.21, 0.46)). However, this association was not significant in univariable (1.64 (0.83, this website 3.24) comparing 3TC to FTC- episodes) or multivariable

analyses (1.55 (0.78, 3.08) comparing 3TC to FTC- episodes). The association between current CD4 count and detection of M184V was also non-significant in multivariable analyses, though episodes in which the most recent viral load was detectable were more likely to result in the detection of M184V (4.20 (1.88, 9.3) comparing viral load >50 copies/ml to viral load ≤50 copies/ml). Patients of black ethnicity were more likely to develop M184V (2.86 (1.44, 5.68) compared with patients of white ethnicity (p = 0.003)). No other factors were significantly associated with the detection of M184V ( Table 2). Forty-eight episodes were followed by the detection of either K65R or M184V, over the course of 9955 person-years, giving an overall event rate of 0.48 (0.35, Rucaparib 0.62)/100 PYFU. Eleven patients developed both M184V and K65R mutations. The overall event

rate for 3TC-episodes was 0.69 (0.38, 1.13)/100 PYFU, whilst the overall event rate for FTC-episodes was 0.49 (0.33, 0.65)/100 PYFU. The univariable relative rate comparing 3TC-episodes to FTC episodes was non-significant (1.61 (0.87, 2.97)). Similarly, after adjusting for potential confounders (Table 2), no association was seen between type of regimen and detection of K65R or M184V (1.43 (0.77, 2.66)). Lower current CD4 counts (1.73 (0.91, 3.26) comparing ≤200 cells to >350 cells) and higher viral loads (4.53 (2.14, 9.61) comparing viral load >50 copies/ml to viral load ≤50 copies/ml) were both associated with a higher risk of detection of either K65R or M184V. Patients of black ethnicity were also more likely to develop either K65R or M184V (p = 0.

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