of the carcinogenic mechanism for polycyclic aromatic hydrocarbons - extended bay region theory and its quantitative model

1 January 1985

journal article
research article
Published by Oxford University Press (OUP) in Carcinogenesis: Integrative Cancer Research

Vol. 6 (1) , 1-6
https://doi.org/10.1093/carcin/6.1.1

Abstract

With the help of results on the metabolism and the carcinogenic activities of polycyclic aromatic hydrocarbons (PAH), the comprehensive metabolic process in vivo is discussed. It is thought that the carcinogenic activity exhibited by a PAH is determined by the competition between the carcinogenesis and detoxification in which it participates. It is suggested that the essential agent of carcinogenesis should be, as a rule, the highest delocalization energy (β unit) of the carbonium ion at the aromatic angular ring (A region), which is obtained by the perturbational molecular orbit (PMO) method. Since there are no essential distinctions in the molecular geometry and delocalization energy states between two carbonium ions of the aromatic angular ring and of the bay region, the A region can be looked upon as the extended bay region. On the basis of discussion of the overall metabolism, evaluation of the detoxification efficacy of each kind of the competing carcinogenic factors, including the biological factor B and three structural factors of the PAH molecule: K, A and L, was made. After making necessary approximation, K=0.228, A=0.5, L=1.22 and B=0.7 are obtained. It can be seen from these values that the L region plays the most important role in detoxification processes, and the K region plays the least important role. The effect of biological factor B is approximately the sum of the K region and the A region. This paper suggests the concept of a carcinogenic constant. For the PAHs with the same number of aromatic rings (N), C is a constant. The curve of function C=f(N), including the extensional line, is an isosceles triangle. The author suggests that it should be called the ‘Pyramid Rule’. The final form of the quantitative equation is

log R = C [Δ E_{deloc}^{3} / (0.7 + 0.228 n_{k} + 0.5 n_{a} + 1.22 n_{1})]

. The values for 50 PAHs which had been tested by animal experiments were calculated. Of these, 92% of the PAHs are in agreement with experiments on carcinogenic activities.

This publication has 7 references indexed in Scilit:

MUTAGENICITY OF THE DIHYDRODIOLS AND BAY-REGION DIOL-EPOXIDES OF BENZO(C)PHENANTHRENE IN BACTERIAL AND MAMMALIAN-CELLS
1980
TUMORIGENICITY OF THE DIHYDRODIOLS OF DIBENZO(A,H)ANTHRACENE ON MOUSE SKIN AND IN NEWBORN MICE
1979
Mutagenicity and cytotoxicity of benz[ a ]anthracene diol epoxides and tetrahydro-epoxides: Exceptional activity of the bay region 1,2-epoxides
Proceedings of the National Academy of Sciences, 1977
Carcinogenicity of Epoxides, Lactones, and Peroxy Compounds. VI. Structure and Carcinogenic Activity23
JNCI Journal of the National Cancer Institute, 1967
The carcinogenic activities in mice of compounds related to benz[a]anthracene
International Journal of Cancer, 1967
The carcinogenic activities in mice of compounds related to 3‐methylcholanthrene
International Journal of Cancer, 1967
Low Carcinogenicity of the K-Region Epoxides of 7-Methylbenz(a)-anthracene and Benz (a) anthracene in the Mouse and Rat.
Experimental Biology and Medicine, 1967