2
15. 1. 1978 Specialia 85 External features (34 experimental and 34 control embryos) Histological observations (26 experimentals and 26 controls) Very Good Re- Dead Vesicle Body Tail CNS Heart Liver good tarried diameter length length abnormal abnormal normal small absent Experi- 5 15 5 9 2.97 4- 1.97 4- 1.75 4- 12 5 .... 8 12 6 mentals 0.067 0.079 0.077 Controls 24 6 1 3 3.44 4- 2.49 4- 2.32 4- 9 4 24 1 1 0.079 0.070 0.088 Vesicle, body and tail measurements are in mm, 4- SE; other figures represent numbers of embryos in each category. streptozotocin has deleterious effects on the growth and viability of embryos at this stage. The apparently delayed development of the liver may be linked with the failures in yolk sac circulation, since the liver develops from the proximal anterior wall of the yolk sac and is also a site of haemopoiesis. None of these effects, however, parallels the abnormalities that have so far been observed in embryos of streptozotocin-diabetic rats (i.e. mal- formations of the nervous system and heart, skeletal deficiencies and exomphalosT). So it seems likely that these latter abnormalities were attributable to the maternal diabetes rather than to any direct effects of streptozotocin. Moreover, since the female rats were injected with streptozotocin either before mating or on day 0, and it is eliminated from the body within 4-6 h 3, only early cleavage stages of embryos could be at much risk of exposure to the drug. The present work shows, however, that administration of streptozotocin to rats at post-implantation stages of pregnancy could have severe effects on the further development of the embryos. Modification of hepatotoxic effects of aflatoxin B 1 in rabbits by immunization 1 I. Ueno 2 and F. S. Chu 3 Food Research Institute and Department o/ Food Microbiology and Toxicology, University o/ Wisconsin, Madison (Wisconsin 53706, USA), 6 June 7977 Summary. Reduction of acute toxic effect of aflatoxin B 1 was achieved by immunizing the rabbits with small amounts of bovine serum albumin-aflatoxin B~ conjugate. Rabbits after immunization showed lower mortality, near normal serum isocitric dehydrogenase activity, no abnormality in livers when challenged with a single dose of aflatoxin B1. The results suggest that immunization might be used prophylactically against aflatoxicosis. Aflatoxin B 1 (aria B1) is one of the most potent environ- mental carcinogens and hepatotoxins produced by Aspergillua parasiticus and A. /lavus. Because of the potential hazard of this toxin to human and animal health, the chemistry and the biochemical and pathologi- cal effects of afla B 1 have been studied extensively in the last decade 4,5. Unlike most bacterial toxins, afla B~ and other mycotoxins are small molecular weight fungal metabolites with diverse chemical structures. While these toxins are devoid of any antigenicity, an aria Bl-l-(0-carboxymethyl)-oxime can be prepared through derivation s,7. The new derivative has a carboxyl group which is readily coupled to a protein for immunization. Using this approach, investigators in this and other laboratories 7, 8 have produced antibody in rabbits sbowing high affinity to afla B~ after the animals were immunized with either bovine serum albumin (BSA)-alIa B 1 con- jugate or with polylysine-afla B 1 conjugate. The antibody was also found to be useful in the radioimmunoassay for afla B,. The present study was carried out in order to find whether or not immunization might be used pro- phylactically against afiatoxicosis. Material and methods. Since rabbits are among the most sensitive animals with regard to afla B~ toxicity, this species was selected for study. Albino female rabbits weighing 3.5 kg were divided into 6 groups of 3 7 rabbits each. 3 groups of rabbits were immunized with BSA-afla B 1 conjugate (210 ~xg per rabbit) which contained 13 moles of aria B~/mole of BSA, according to the method previously described 8. Rabbits in the other 3 groups were raised under the same conditions but were not immunized. Antibody titers of the immunized rabbits were determined by a binding method9 every week starting from the 4th week after immunization. 6 weeks after immunization, all the animals were challenged with a single dose of pure alfa B 1 by i.p. injection. Mortality and serum isocitric dehydrogenase activity (ICDH, Sigma method 1~ were monitored. Limited histological examinations on 1 Supported by the College of Agricultural and Life Sciences, the University of Wisconsin, by Public Health Service research grant number CA 15064 from the National Cancer Institute, and by contribution from food industries to the Food Research Institute of University of Wisconsin. 2 Visiting scientist from University of Tokyo, Tokyo, Japan. 3 The authors wish to thank Prof. R. D. Hinsdill for his comments during the preparation of the manuscript. 4 L.A. Goldblatt, Aflatoxin - Scientific background, control and implications. Academic Press, New York 1969. 5 G.N. Wogan, A. Rev. Pharmac. 75, 437 (1975). 6 F.S. Chu, M. T. Stephen Hsia and Piera Sun, J. Ass. off. analyt. Chem. 60, 791 (1977). 7 J.J. Langone and H. Van Vunakis, J. natl. Cancer Inst. 56, 591 (1976). 8 F.S. Chu and I. Ueno, Appl. environ. Mierobiol. 33, 1125 (1977). 9 F.S. Chu, Fred C. C. Chang and R. D. Hinsdill, Appl. environ. Microbiol. 31, 831 (1976/. 10 E. Bernt and H. U. Bergmeyer, in: Methods of enzymatic analysis, p. 624. Ed. H. U. Bergmeyer. Academic Press, New York; and Sigma technical bulletin number 175/150.

Modification of hepatotoxic effects of aflatoxin B1 in rabbits by immunization

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Page 1: Modification of hepatotoxic effects of aflatoxin B1 in rabbits by immunization

15. 1. 1978 Specialia 85

External features (34 experimental and 34 control embryos) Histological observations (26 experimentals and 26 controls) Very Good Re- Dead Vesicle Body Tail CNS Heart Liver good tarried diameter length length abnormal abnormal normal small absent

Experi- 5 15 5 9 2.97 4- 1.97 4- 1.75 4- 12 5 .... 8 12 6 mentals 0.067 0.079 0.077

Controls 24 6 1 3 3.44 4- 2.49 4- 2.32 4- 9 4 24 1 1 0.079 0.070 0.088

Vesicle, body and tail measurements are in mm, 4- SE; other figures represent numbers of embryos in each category.

s t r ep tozo toc in has deleter ious effects on the g rowth and v iabi l i ty of embryos a t th is stage. The a p p a r e n t l y delayed d e v e l o p m e n t of the l iver m a y be l inked wi th the failures in yolk sac circulat ion, since the liver develops f rom the p rox imal an te r ior wall of the yolk sac and is also a site of haemopoiesis . None of these effects, however , paral lels the abnormal i t i es t h a t have so far been observed in embryos of s t rep tozo toc in -d iabe t i c ra t s (i.e. mal- fo rma t ions of t he nervous sys t em and hear t , skeletal deficiencies and exomphalosT). So it seems likely t h a t

these l a t t e r abnormal i t i es were a t t r i bu t ab l e to the ma t e rn a l d iabetes r a the r t h a n to any di rect effects of s t rep tozotoc in . Moreover, since the female ra t s were in jec ted wi th s t rep tozo toc in e i ther before ma t ing or on day 0, and i t is e l imina ted f rom the body wi th in 4-6 h 3, only early cleavage s tages of embryos could be a t m u c h risk of exposure to the drug. The p resen t work shows, however , t h a t admin i s t r a t ion of s t r ep tozo toc in to ra t s a t p o s t - i mp l an t a t i o n s tages of p r e g n a n c y could have severe effects on the fu r the r d e v e l o p m e n t of the embryos .

M o d i f i c a t i o n of h e p a t o t o x i c e f fec ts of a f l a t o x i n B 1 in r a b b i t s b y i m m u n i z a t i o n 1

I. Ueno 2 and F. S. Chu 3

Food Research Institute and Department o/ Food Microbiology and Toxicology, University o/ Wisconsin, Madison (Wisconsin 53706, USA), 6 June 7977

Summary. Reduc t ion of acute toxic effect of af la toxin B 1 was achieved by immuniz ing the r abb i t s w i th small amo un t s of bovine se rum a lbumin-a f l a tox in B~ conjugate . R a b b i t s af ter immun iza t i on showed lower mor ta l i ty , near no rma l se rum isocitric dehydrogenase act iv i ty , no abno rma l i t y in livers when chal lenged wi th a single dose of a f la toxin B1. The resul ts suggest t h a t immuniza t ion migh t be used p rophy lac t i ca l ly agains t aflatoxicosis .

Af la tox in B 1 (aria B1) is one of the mos t p o t e n t envi ron- men ta l carc inogens and hepa to tox in s p roduced by Aspergillua parasiticus and A. /lavus. Because of the po ten t i a l hazard of th is tox in to h u m a n and an imal hea l th , the chemis t ry and the biochemical and pa thologi - cal effects of afla B 1 have been s tudied ex tens ive ly in the last decade 4,5. Unlike mos t bacter ia l toxins , afla B~ and o the r myco tox ins are small molecular weight fungal me tabo l i t e s with diverse chemical s t ruc tures . Whi le these toxins are devo id of any ant igenic i ty , an aria B l - l - (0 - ca rboxyme thy l ) -ox ime can be p repa red t h ro u g h de r iva t ion s,7. The new der iva t ive has a ca rboxyl group which is readi ly coupled to a p ro te in for immuniza t ion . Us ing th is approach , inves t iga tors in th is and o the r laborator ies 7, 8 have p roduced an t i body in rabb i t s sbowing high af f in i ty to afla B~ af ter the animals were immunized wi th e i ther bovine serum a lbumin (BSA)-alIa B 1 con- juga te or w i th polylys ine-af la B 1 conjugate . The a n t i b o d y was also found to be useful in the r ad io immunoas s ay for afla B,. The p re sen t s t u d y was carried ou t in order to f ind w h e t h e r or no t immuniza t ion migh t be used pro- phy lac t i ca l ly agains t afiatoxicosis. Material and methods. Since rabb i t s are among the mos t sensi t ive animals w i th regard to afla B~ toxic i ty , th is species was selected for s tudy. Albino female r abb i t s weighing 3.5 kg were d iv ided into 6 groups of 3 7 r abb i t s each. 3 groups of r abb i t s were immunized wi th BSA-af la B 1 conjuga te (210 ~xg per rabbi t) which con ta ined 13 moles of aria B~/mole of BSA, according to the m e t h o d previous ly

descr ibed 8. R a b b i t s in t he o the r 3 groups were raised under the same condi t ions b u t were no t immunized . A n t i b o d y t i te rs of the immunized rabb i t s were de t e rmined by a b ind ing method9 every week s ta r t ing f rom the 4 th week af ter immuniza t ion . 6 weeks af ter immuniza t ion , all the animals were chal lenged with a single dose of pure alfa B 1 by i.p. inject ion. Mor ta l i ty and serum isocitric dehydrogenase ac t iv i ty (ICDH, Sigma m e t h o d 1~ were moni tored . L imi ted his tological examina t ions on

1 Supported by the College of Agricultural and Life Sciences, the University of Wisconsin, by Public Health Service research grant number CA 15064 from the National Cancer Institute, and by contribution from food industries to the Food Research Institute of University of Wisconsin.

2 Visiting scientist from University of Tokyo, Tokyo, Japan. 3 The authors wish to thank Prof. R. D. Hinsdill for his comments

during the preparation of the manuscript. 4 L.A. Goldblatt, Aflatoxin - Scientific background, control and

implications. Academic Press, New York 1969. 5 G.N. Wogan, A. Rev. Pharmac. 75, 437 (1975). 6 F.S. Chu, M. T. Stephen Hsia and Piera Sun, J. Ass. off. analyt.

Chem. 60, 791 (1977). 7 J . J . Langone and H. Van Vunakis, J. natl. Cancer Inst. 56,

591 (1976). 8 F.S. Chu and I. Ueno, Appl. environ. Mierobiol. 33, 1125 (1977). 9 F.S. Chu, Fred C. C. Chang and R. D. Hinsdill, Appl. environ.

Microbiol. 31, 831 (1976/. 10 E. Bernt and H. U. Bergmeyer, in: Methods of enzymatic

analysis, p. 624. Ed. H. U. Bergmeyer. Academic Press, New York; and Sigma technical bulletin number 175/150.

Page 2: Modification of hepatotoxic effects of aflatoxin B1 in rabbits by immunization

86 Specialia EXPERIENTIA 34/1

Effect of immunizationon the susceptibilityofrabbits to aflatoxin BI*

AflaB 1 dose (mg/rabbit)

Mortality (No. of deaths/surviving) Control Immunized

0.75 3/7 0/7 1.0 2/4 0/4 0.75 -t- 1.50"* 2/3 2/3

* Rabbit size was 3.5 kg. Mortality was recorded in 2-7 days after a single dose of i.p. injection with pure aria B 1. **Challenged with 0.75 mg first and then again with 1.5 mg afla B 1 17 days after the first injection.

I

E

g >-

- 1 - r

i i 1 1

1 2 3 4 5

Days after injection

Fig. 1. Serum isoeitric dehydrogenase activity of the immunized (-O-O-) and nonimmunized (--0-0-) rabbits after receiving a single dose (0.75 mg/rabbit) of aflatoxin B 1.

80 '

60

40

5 5

20

0~ 8

Days before and after injection

Fig. 2. Binding capacity of rabbit antiserum with 3H-afla B 1 before and after rabbits received a single dose (0.75 mg/rabbit) of aflatoxin B x. All serum was precipitated with (NHa)~SO 4 at 33% saturation and a final dilution of 1 : 500 was made prior to assay. Representation of experimental results from 4 rabbits is presented.

t he l ivers of the dead a n d s u r v i v i n g r a b b i t s were k i n d l y p e r f o r m e d b y Prof. J . R. Al ien of t he P a t h o l o g y D e p a r t - m e n t , U n i v e r s i t y of Wiscons in -Madison . Results and discussion. The effects of i m m u n i z a t i o n on t h e m o r t a l i t y of cha l l enged r a b b i t s are s u m m a r i z e d in t he tab le . W h e n r a b b i t s were cha l l enged w i t h af la B x a t LDs0 or s l igh t ly h i g h e r dosages (LDs0 of af la t31 = 0.3 mg/kg) , all t h e i m m u n i z e d r a b b i t s were p ro t ec t ed f rom t h e acu te toxic effect. In con t r a s t , t h e expec ted m o r t a l i t y r a t e was obse rved in t he u n i m m u n i z e d con t ro l r abb i t s . P r o t e c t i o n is n o t abso lu te , however , s ince i m m u n i z e d r a b b i t s cha l l enged w i t h r o u g h l y a 2 LDs0 dose 17 days a f t e r the f i rs t cha l lenge showed a h ighe r t h a n 50% m o r t a l i t y . The p r o t e c t i v e effect of i m m u n i z a t i o n was also e v i d e n t f rom the s e rum I C D H tes t s a n d h is to logica l e x a m i n a t i o n s . F igu re 1 shows t h a t t he s e r u m I C D H a c t i v i t y in t he con t ro l r a b b i t s increased s ign i f i can t ly a f t e r t h e y received af la B 1 (0.75 mg / r abb i t ) , whereas t he enzyme a c t i v i t y of i m m u n i z e d r a b b i t s e r u m increased on ly s l igh t ly above n o r m a l range. His to logica l e x a m i n a t i o n s of t he r a b b i t l ivers revea led t h a t t he con t ro l r a b b i t s d ied f rom a t yp i ca l af la toxicosis , inc lud ing a c e n t r i l o b u l a r necrosis, a n d f a t t y i n f i l t r a t i on in the liver. The l ivers of i m m u n i z e d r a b b i t s w h i c h su rv ived t he cha l lenge showed no a b n o r m a l i t y . I n order to d e t e r m i n e w h e t h e r t he p r o t e c t i v e effect was due to t he i n t e r ac t i on of af la B 1 w i t h an t i - a l i a B 1 an t i - body , t he b ind ing c a p a c i t y of r a b b i t s e rum w i t h 3H-afla B~ was m o n i t o r e d t h r o u g h o u t t he expe r imen t s . F igure 2 shows t h a t t he b ind ing c a p a c i t y decreased r ap id ly a f t e r t h e r a b b i t s received t he cha l lenge w i t h un labe l l ed af la Bx b u t r e t u r n e d to n e a r n o r m a l levels 3-4 days a f t e rwards . T h e resu l t s ind ica te t h a t i m m e d i a t e l y a f t e r t h e an ima l s rece ived t he myco tox in , t he b ind ing s i tes of t he s e rum a n t i b o d y were occupied b y t h e un labe l l ed afla 131; as soon as t he t ox in lef t t he b loods t r eam, pe rhaps t h r o u g h excre t ion , t he new b i n d i n g si tes which are p r o b a b l y loca ted in t he newly syn thes i zed a n t i b o d y , became avai l - ab le for the in v i t ro b i n d i n g w i t h 3H-afla 131. R a b b i t s in t he 3 group, wh ich showed l i t t l e p r o t e c t i o n w h e n cha l l enged a second t i m e w i t h af la B 1 (2 LDs0 dose), m a y h a v e h a d insuf f ic ien t a n t i b o d y to b i n d and neu t ra l i ze t h e toxin . I t is also i n t e r e s t i ng to specula te t h a t since m e t a b o l i s m plays a n i m p o r t a n t role for afla B 1 toxic i ty , i n t e r a c t i o n of afla B 1 w i t h homologous a n t i b o d y could h i n d e r t h e a c t i v a t i o n of af la B 1 to a n ac t ive molecule, t h u s p r e v e n t i n g t he m a n i f e s t a t i o n of t he toxic effects. The p r e sen t s t u d y ind ica t e s t h a t i t is possible to increase t h e res i s t ance in an ima l s to af la toxicos is b y i m m u n i z a - t ion , b u t i t is no t k n o w n w h e t h e r i m m u n i z a t i o n m i g h t i n h i b i t t he af la 13x induced hepa toca rc inogen ic effect in an imals . Peck and Peck 1~ sugges ted t h a t i m m u n i z a t i o n m i g h t be a p r ac t i c a l m e a n s to p r e v e n t cancer in h u m a n s . I n t h e i r s t u d y of t u m o r i n d u c t i o n in r a t s w i th 2 - a n t h r y l - amine , t h e y d e m o n s t r a t e d t h a t a 50% inh ib i t i on of t u m o r f o r m a t i o n was ach i eved b y i m m u n i z i n g Sprague- D a w l e y female r a t s w i t h 2 - a n t h r y l a m i n o h u m a n s e r u m a lbumin -41 conjuga te . Therefore , i t is possible t h a t t he carc inogenic effect of af la B 1 m i g h t also be i nh ib i t ed a f t e r i m m u n i z a t i o n . S tudies in our l a b o r a t o r y are c u r r e n t l y d i r ec ted to ver i fy such a poss ib i l i ty . Since we h a v e used on ly a one-s tep mul t iP le s i tes i n j ec t i on m e t h o d for i m m u n i z a t i o n , c o n t i n u o u s boos t ing of t h e an ima l s w i t h BSA-a I l a B 1 c o n j u g a t e would l ike ly p roduce h i g h e r a n t i b o d y t i t e r s and t h u s t h e g rea te r p ro t ec t i ve effect. I m p r o v e d m e t h o d s for i m m u n i z a t i o n w a r r a n t f u r t h e r i nves t iga t ion .

11 R.M. Peck and E. B. Peck, Cancer Res. 31, 1550 (1971).