The Distribution and Excretion of 2,4,5,2',5'-pentachlorobiphenyl in the Rat

Overview

Journal Drug Metab Dispos

Specialty Pharmacology

Date 1975 May 1

PMID 238820

Citations 19

Authors

H B Matthews

M W Anderson

Affiliations

Soon will be listed here.

Abstract

Rats received single intravenous doses (0.6 or 6.0 mg/kg) of 2,4,5,2',5'-pentachlorobiphenyl-14C (5-CB). The distribution and ecretion of 5-CB-derived material were investigated at periods ranging from 10 min to 42 days after administration and found to be first-order rate processes in the dose range studied. Blood, liver, muscle, skin, and adipose tissues were found to be the most important tissues to the distribution of this compound. More than 90% of the total dose was removed from the blood within 10 min after administration. Most of the radioactivity was initially deposited in the liver and muscle, and then translocated to the skin and adipose tissue. The decay rate of radioactivity from each of the tissues could be described by the sum of two or more exponentials. Metabolism to more polar compounds appears to be a prerequisite to excretion, and most of the radioactivity was excreted in the bile and ultimately in the feces. Excretion in the urine accounted for less than 7% of the total dose and ceased at approximately 8 or 9 days after 5-CB-administration. Studies of the distribution and excretion of 5-CB-derived material over extended periods of time, 1-42 days, demonstrated the importance of the adipose tissue and skin as long-term storage sites, and demonstrated that the decay rate of 5-CB from the tissues paralleled the decreasing rate of excretion in the feces.

Citing Articles

Predictors of plasma polychlorinated biphenyl concentrations among reproductive-aged black women.

Wesselink A, Bethea T, McClean M, Weuve J, Williams P, Hauser R Int J Hyg Environ Health. 2019; 222(7):1001-1010.

PMID: 31285139 PMC: 6684292. DOI: 10.1016/j.ijheh.2019.06.008.

Transgenerational effects of polychlorinated biphenyls: 1. Development and physiology across 3 generations of rats.

Mennigen J, Thompson L, Bell M, Santos M, Gore A Environ Health. 2018; 17(1):18.

PMID: 29458364 PMC: 5819226. DOI: 10.1186/s12940-018-0362-5.

Prenatal PCBs disrupt early neuroendocrine development of the rat hypothalamus.

Dickerson S, Cunningham S, Gore A Toxicol Appl Pharmacol. 2011; 252(1):36-46.

PMID: 21277884 PMC: 3060304. DOI: 10.1016/j.taap.2011.01.012.

Endocrine disruption of brain sexual differentiation by developmental PCB exposure.

Dickerson S, Cunningham S, Patisaul H, Woller M, Gore A Endocrinology. 2010; 152(2):581-94.

PMID: 21190954 PMC: 3037168. DOI: 10.1210/en.2010-1103.

Minding the calcium store: Ryanodine receptor activation as a convergent mechanism of PCB toxicity.

Pessah I, Cherednichenko G, Lein P Pharmacol Ther. 2009; 125(2):260-85.

PMID: 19931307 PMC: 2823855. DOI: 10.1016/j.pharmthera.2009.10.009.