. Author manuscript; available in PMC: 2016 Jun 10.

Published in final edited form as: J Med Chem. 2015 Aug 4;58(15):5863–5888. doi: 10.1021/acs.jmedchem.5b00423

Table 6.

In Vivo PK Data for Analogue 33 Following IV and PO Administration in Rats^a

route	dose (µmol/kg)	C₀^b (µM)	CL^c (mL/h/kg)	t_1/2^d (h)	V_ss^e (mL/kg)	AUC_last^f (µM·h)	AUC_INF^g (µM·h)	%Fⁱ
IV	5.1	58.6 (1.8)	5.06 (0.49)	22.0 (3.0)	156 (9.0)	795 (48)	1017 (93)	NA

route	dose (µmol/kg)	C_max^h (µM)	T_max^h (h)	t_1/2^d (h)	V_ss^e (mL/kg)	AUC_last^f (µM·h)	AUC_INF^g (µM·h)	%Fⁱ

PO	12.7	62.2 (4.3)	2.67 (1.15)	38.8 (17.3)	NA	2011 (326)	3636 (1588)	143 (62.4)

Data are represented as the mean with standard deviation in parentheses (mean (SD)). Dosing groups consisted of three drug naïve adult male Sprague–Dawley rats. IV administration: the test article was administered at the 5.1 µmol/kg (2 mg/kg) dose; test article vehicle = 3% DMA/45% PEG300/12% EtOH/40% sterile H₂O; PO administration, test article was administered at the 12.7 µmol/kg (5 mg/kg) dose; vehicle = 2% Tween 80 in 0.9% saline. Bioavailability; F = (AUC_INFpo × dose_iv) ÷ AUC_INFiv × dose_po).

Observed initial concentration of compound in plasma at time zero.

Total body clearance.

Apparent half-life of the terminal phase of elimination of the compound from plasma.

Volume of distribution at steady state.

Area under the plasma concentration versus time curve from 0 to the last time point that the compound was quantifiable in plasma.

Area under the plasma concentration versus time curve from 0 to infinity.

Maximum observed concentration of the compound in plasma.

ⁱ

Time of maximum observed concentration of the compound in plasma.