Biodistribution, pharmacokinetics and toxicity of a Vasconcellea cundinamarcensis proteinase fraction with pharmacological activity

Lemos, Fernanda O.; Villalba, Maria Imaculada C.; Tagliati, Carlos A.; Cardoso, Valbert N.; Salas, Carlos E.; Lopes, Miriam T.P.

doi:10.1016/j.bjp.2015.09.008

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Original Article • Rev. bras. farmacogn. 26 (1) • Jan-Feb 2016 • https://doi.org/10.1016/j.bjp.2015.09.008 copy

Biodistribution, pharmacokinetics and toxicity of a Vasconcellea cundinamarcensis proteinase fraction with pharmacological activity

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Prior studies demonstrate that a proteinase fraction from Vasconcellea cundinamarcensis V.M. Badillo, Caricaceae, exhibits wound healing activity in gastric and cutaneous models and antitumoral/antimetastatic effects. Here, we present the toxicity, pharmacokinetics and biodistribution data for this proteinase fraction following a single dose into Swiss mice by i.v., s.c. or p.o. routes. The i.v. and s.c. toxicity assays demonstrate that proteinase fraction at ≤20 mg/kg is non-lethal after single injection, while parental administration (p.o.) of ≤300 mg/kg does not cause death. Based on p.o. acute toxicity dose using Organisation for Economic Cooperation and Development protocols, proteinase fraction ranks as Class IV “harmful” substance. Proteinase fraction shows high uptake determined as Kp (distribution tissue/blood) in organs linked to metabolism and excretion. Also, high bioavailability (≈100%) was observed by s.c. administration. The blood contents following i.v. dose fits into a pharmacokinetic bi-compartmental model, consisting of high removal constants – k_el 0.22 h⁻¹ and k_d 2.32 h⁻¹and a half-life – t_½ = 3.13 h. The Ames test of proteinase fraction (0.01–1%) demonstrates absence of mutagenic activity. Likewise, genotoxic evaluation of proteinase fraction (5 or 10 mg/kg, i.p.) shows no influence in micronuclei frequency. In conclusion, the acute doses for proteinase fraction lack mutagenic and genotoxic activity, clearing the way for clinical assays.

Keywords
Caricaceae; Cysteine proteinases; Biodistribution; Pharmacokinetics; Toxicity

Organ	Administration routes
	i.v.		s.c.		p.o.
	AUC	Kp	AUC	Kp	AUC	Kp
Blood	10.9	1.0	12.1	1.0	0.9	1.0
Liver	45.2	4.1	19.2	1.6	2.1	2.3
Spleen	12.7	1.2	6.5	0.5	0.7	0.8
Stomach	7.9	0.7	5.3	0.4	292.2	323.9
Small intestine	12.3	1.1	11.9	1.0	55.0	61.0
Large intestine	57.2	5.2	30.9	2.6	400.6	444.1
Kidney	504.9	46.3	490.9	40.7	5.6	6.2
Bladder/urine	1192.0	109.3	1263.0	104.6	29.4	32.6
Thyroid	5.7	0.5	8.3	0.7	1.5	1.6
Fat	3.5	0.3	3.1	0.3	0.3	0.4
Brain	0.6	0.1	1	0.1	0.1	0.1
Heart	6.9	0.6	6.7	0.6	0.6	0.7
Lung	10.7	1.0	8.7	0.7	0.7	0.8
Skin	7.8	0.7	7.5	0.6	1.6	1.8

Pharmacokinetic parameters
k_d (h⁻¹)	2.32 ± 1.03
k_el (h⁻¹)	0.22 ± 0.20
t_½ distribution (h)	0.29 ± 0.67
t_½ elimination (h)	3.13 ± 3.42
AUC (% dose/ml × h)	10.9
Oral bioavailability (%)	8.3
Subcutaneous bioavailability (%)	111

Route	Dose (mg/kg)	T/D	T/P	Clinical signs
i.v.	Control	5/0	(−)	(−)
	5	5/0	5/2	Phlebitis (+) Remission 7–12 days
	10	5/0	5/3	Phlebitis (++) Remission 7–12 days
	20	5/0	5/5	Phlebitis (+++) Remission 7–14 days

s.c.	Control	5/0	(−)	(−)
	5	5/0	(−)	(−)
	10	5/0	5/2	Cutaneous lesion (++) Remission in 9 days
	20	5/0	5/5	Cutaneous lesion (+++) Remission 9–14 days

p.o.	Control	5/0	(−)	(−)
	5	5/0	(−)	(−)
	10	5/0	(−)	(−)
	300	5/0	(−)	(−)

Treatment (mg/plate)	Revertant colonies (mean ± SD)
	TA98		TA100		TA97		TA102
	−S9	+S9	−S9	+S9	−S9	+S9	−S9	+S9
Negative control (H ₂ O)	21.7 ± 4.1	25.0 ± 5.4	165.3 ± 27.1	155.3 ± 25.5	171.7 ± 19.4	138.3 ± 11.4	126.7 ± 15.8	133.3 ± 18.9

P1G10
0.1 mg (MR)	31.3 ± 1.8 (1.4)	24.3 ± 3.4 (0.9)	81.3 ± 17.4 (0.5)	66.7 ± 2.9 (0.4)	134.7 ± 27.5 (0.8)	100.3 ± 3.2 (0.72)	77.0 ± 1.2 (0.6)	128.0 ± 24.7 (1.0)
1.0 mg (MR)	19.3 ± 3.4 (0.9)	23.3 ± 2.4 (0.9)	88.0 ± 17.3 (1.0)	105.3 ± 10.4 (1.6)	128.7 ± 52.9 (0.7)	64.3 ± 4.0 (0.5)	107.0 ± 1.2 (0.8)	155.0 ± 3.9 (1.2)
10 mg (MR)	15.3 ± 2.4 (0.7)	27.3 ± 0.3 (1.1)	124.0 ± 25.7 (0.7)	117.3 ± 12.6 (0.7)	94.7 ± 1.1 (0.5)	29.3 ± 2.9 (0.2)	69.7 ± 3.5 (0.5)	166.7± 11.1 (1.2)

Positive control (MR)	132.9 ± 32.9 ^* * p < 0.05 ANOVA, Bonferroni post-test. (6.2)	118.6 ± 22.0 (4.7)	1211.9 ± 112.6 ^* * p < 0.05 ANOVA, Bonferroni post-test. (7.3)	1561.3 ± 121.1 ^* AUC, area under the curve; Kp, partition coefficient; Administration routes: i.v. , intravenous; s.c. , subcutaneous; p.o. , oral. Dose: 1 mg/kg 99mTc-P1G10. Radioactive dose = 3 mBq. (10.0)	861.33 ± 174.74 ^* * p < 0.05 ANOVA, Bonferroni post-test. (5.0)	278.6 ± 106.9 ^* AUC, area under the curve; Kp, partition coefficient; Administration routes: i.v. , intravenous; s.c. , subcutaneous; p.o. , oral. Dose: 1 mg/kg 99mTc-P1G10. Radioactive dose = 3 mBq. (2.1)	1976.6 ± 159.2 ^* * p < 0.05 ANOVA, Bonferroni post-test. (15.6)	1799.6 ± 154.1 ^* * p < 0.05 ANOVA, Bonferroni post-test. (13.5)

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[1] * Corresponding author. cesbufmg@icb.ufmg.br