Dinocap Dermal Absorption in Female Rabbits and Rhesus Monkeys

Dec 23, 1988 - The dermal absorption of dinocap was determined in female rabbits and rhesus monkeys as part of the risk assessment for KarathaneR ...
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Chapter 11

Dinocap Dermal Absorption in Female Rabbits and Rhesus Monkeys Implications for Humans Downloaded by UNIV OF MASSACHUSETTS AMHERST on May 30, 2018 | https://pubs.acs.org Publication Date: December 23, 1988 | doi: 10.1021/bk-1988-0382.ch011

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Stephen L. Longacre , Laura J. DiDonato , Ronald C. Wester , Howard I. Maibach , Susan S. Hurt , and Richard D. Costlow 2

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Toxicology Department, Rohm and Haas Company, Spring House, PA 19477 Department of Dermatology, University of California School of Medicine, San Francisco, CA 94143

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The dermal absorption of dinocap was determined in female rabbits and rhesus monkeys as part of the risk assessment for Karathane Fungicide/Miticide. C-2,4-Dinitro-6-(1-methylheptyl)phenyl crotonate (2,4-DNHPC) was used as the model isomer for dinocap in these studies. In r a b b i t s , the dermal absorption of 25 mg/kg (approximately 2500 ug/cm ) 2,4-DNHPC was 4-9%, whether 2,4-DNHPC was applied neat (undiluted) or dissolved in acetone, or applied as the wettable powder or l i q u i d concentrate formulation. The total absorption of 13 d a i l y 6-hr dermal doses of 25 mg/kg/day (2500 ug/cm /day) of neat 2,4-DNHPC in rabbits was 6%, similar to the percent absorption observed following a single dermal dose. In rhesus monkeys, the dermal absorption of 2,4-DNHPC at 2500 ug/cm (in acetone) was similar to the dermal absorption in rabbits (5%). Dermal absorption of 2,4-DNHPC in monkeys at 40 ug/cm was 16%; this dose approxmated a u s e - d i l u t i o n . The absorption data for 2,4-DNHPC in rabbits and monkeys support the conclusion that, under expected use conditions, dermal exposure to dinocap does not pose an unreasonable developmental r i s k to man. R

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Dinocap (Karathane Fungicide/Miticide) was registered by Rohm and Haas Company in the United States in 1951, and is p r i n c i p a l l y used as a fungicide for control of powdery mildew and as a m i t i c i d e . Dinocap contains as i t s active ingredients a mixture of 2,4- and 2,6-dinitrooctylphenyl crotonates in an approximate 2:1 r a t i o , where "octyl" refers to a mixture of 1-methylheptyl, 1-ethylhexyl, NOTE: A more detailed version of these data will be published in a toxicology journal. 0097-6156/89/0382-0137$06.00/0 © 1989 American Chemical Society

Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

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and 1 - p r o p y l p e n t y l i s o m e r s ( F i g u r e 1 ) . S m a l l amounts o f t h e c o r r e s p o n d i n g f r e e p h e n o l s a r e a l s o p r e s e n t as a c t i v e i n g r e d i e n t s . D e v e l o p m e n t a l t o x i c i t y s t u d i e s i n New Z e a l a n d w h i t e r a b b i t s i n d i c a t e d that oral exposure to dinocap t e c h n i c a l during the p e r i o d o f o r g a n o g e n e s i s p r o d u c e d t e r a t a , w h i c h were m a n i f e s t e d as h y d r o ­ c e p h a l u s and/or m a l f o r m a t i o n s o f t h e n e u r a l t u b e and s k u l l ( 1 ) . The n o - o b s e r v e d e f f e c t l e v e l (NOEL) and t h e minimum e f f e c t l e v e l (MEL) f o r d i n o c a p o r a l d e v e l o p m e n t a l t o x i c i t y i n r a b b i t s were j u d g e d t o be 0.5 and 3 mg/kg/day, r e s p e c t i v e l y ( 1 ) . R e s i d u e s o f d i n o c a p on c r o p s a r e s u c h t h a t t h e r i s k o f d i n o c a p t o humans by t h e o r a l r o u t e i s n e g l i g i b l e . To a s c e r t a i n t h e p o s s i b l e r i s k o f dinocap to a g r i c u l t u r a l workers, s e v e r a l s t u d i e s were p e r f o r m e d . T h e s e s t u d i e s i n c l u d e d a d i n o c a p d e r m a l / o r a l a b s o r p t i o n s t u d y i n r a b b i t s , and a d i n o c a p dermal a b s o r p t i o n s t u d y i n r h e s u s monkeys. Our o b j e c t i v e s i n t h e s e a b s o r p t i o n s t u d i e s were a) t o compare t h e p e r c e n t dermal a b s o r p t i o n o f d i n o c a p i n t h e r a b b i t and r h e s u s monkey a t dose l e v e l s used i n r a b b i t d i n o c a p t o x i c o l o g y s t u d i e s , and b) t o d e t e r m i n e t h e p e r c e n t dermal a b s o r p t i o n i n t h e r h e s u s monkey a t p o t e n t i a l worker e x p o s u r e c o n c e n t r a t i o n s . To f a c i l i t a t e t h e i n t e r p r e t a t i o n o f t h e d a t a , t h e a b s o r p t i o n s t u d i e s were p e r f o r m e d u s i n g C - 2 , 4 - d i n i t r o - 6 ( 1 - m e t h y l h e p t y l ) - p h e n y l c r o t o n a t e (2,4-DNHP'C) as t h e model compound f o r the alkyl s u b s t i t u t e d isomers of dinocap (Figure 2 ) . M a t e r i a l s and Methods T e s t Compounds. C-2,4-DNHPC (7.58 mCi/g; r a d i o p u r i t y = 96.5%; m o l e c u l a r w e i g h t = 256 g / m o l e ) , and n o n r a d i o l a b e l e d 2,4-DNHPC p u r i t y = 97%) used t o d i l u t e t h e s p e c i f i c a c t i v i t y o f t h e 4C-2,4-DNHPC, were b o t h s y n t h e s i z e d a t Rohm and Haas Company ( S p r i n g House, P A ) . The t e s t compounds were l i g h t amber c o l o r e d oils. A n i m a l s . F e m a l e New Z e a l a n d w h i t e r a b b i t s (34-42 weeks o l d ; 2.9-3.9 kg; H a z l e t o n D u t c h l a n d ; Denver, P A ) , and f e m a l e r h e s u s monkeys (5.4-10.7 kg; U n i v e r s i t y o f C a l i f o r n i a a t D a v i s P r i m a t e C e n t e r ; D a v i s , CA) were used i n t h e s e s t u d i e s (3 o r 4 a n i m a l s p e r group). 14 Rabbit Intravenous Study. C-2,4-DNHPC, d i s s o l v e d i n d i m e t h y l s u l f o x i d e (DMSO), was a d m i n i s t e r e d i n t h e j u g u l a r v e i n (0.1 m l / k g ) at 3 mg/kg (3 u C i / k g ) . U r i n e and f e c e s were c o l l e c t e d a t i n t e r v a l s up t o 4 days a f t e r d o s i n g and a n a l y z e d f o r t o t a l ' C - l a b e l . A l l r a b b i t s were h u m a n e l y k i l l e d by an i n t r a c a r d i a c i n j e c t i o n o f e u t h a n a s i a s o l u t i o n (T-61 ; A m e r i c a n H o e c h s t C o r p . , S o m e r v i l l e , NJ). R a b b i t O r a l S t u d i e s . C-2,4-DNHPC, s u s p e n d e d i n aqueous 1% gum t r a g a c a n t h , was a d m i n i s t e r e d by gavage (5 m l / k g ) a t 0.5, 3, o r 25 mg/kg (3-17 u C i / k g ) . U r i n e , f e c e s , and p l a s m a were c o l l e c t e d at i n t e r v a l s up t o 4 days a f t e r d o s i n g and a n a l y z e d f o r ^ C - l a b e l . R a b b i t 6 Hr Dermal E x p o s u r e S t u d i e s . The f u r on t h e d o r s a l s i d e o f e a c h r a b b i t was c l i p p e d t o e x p o s e an a r e a o f a p p r o x i m a t e l y 280 cm 1-3 days p r i o r t o d o s i n g . P l a s t i c c o l l a r s were p l a c e d on e a c h rabbit to prevent preening of the application site.p C-2,4-DNHPC (23-31 u C i / k g ) was a p p l i e d d i r e c t l y o n t o a 5 x 8 cm a r e a o f t h e 14

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Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

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LONGACRE ET AL.

Dinocap Dermal Absorption

F i g u r e 1. S t r u c t u r a l f o r m u l a e o f t h e a c t i v e i n g r e d i e n t components o f d i n o c a p [ 2 , 4 - d i n i t r o o c t y l p h e n y l c r o t o n a t e s ( t o p ) and 2 , 6 - d i n i t r o o c t y l p h e n y l c r o t o n a t e s ( b o t t o m ) ] ; "n" e q u a l s 0, 1, and 2.

F i g u r e 2. S t r u c t u r a l f o r m u l a o f C-2,4-DNHPC; t h e a s t e r i s k s indicate location of the C-label.

Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

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c l i p p e d d o r s a l s i t e as a) t h e n e a t ( u n d i l u t e d ) m a t e r i a l a t 25 ( 2 . 2 ) , 100 ( 8 . 3 ) , and 220 mg/kg ( 1 8 . 3 mg/cra ); b) t h e w e t t a b l e d u s t (WD) f o r m u l a t i o n a t 25 mg a i / k g (2.4 mg/cm ) a p p l i e d as a 2 0 . 4 % a i p a s t e (1:1.3 p a s t e : w a t e r ) a t 0.28 g p a s t e / k g ; c ) t h e l i q u i d c o n c e n t r a t e ( L C ) f o r m u l a t i o n a t 25 mg a i / k g ( 2 . 5 mg/cm a p p l i e d as a 3 9 . 8 % a i s o l u t i o n ( 0 . 0 6 m l / k g ) ; o r d) i n a c e t o n e a t 25 mg/kg (2.2 mg/cm ) a p p l i e d as a 3 9 . 8 % a i s o l u t i o n ( 0 . 0 6 m l / k g ) . S i x ( 6 ) h r a f t e r d o s e a p p l i c a t i o n , t h e a p p l i c a t i o n s i t e s were w i p e d w i t h gauze pads s o a k e d w i t h aqueous 9 5 % e t h a n o l , f o l l o w e d by w i p i n g w i t h pads s a t u r a t e c L w i t h w a t e r . A p p l i c a t i o n s i t e s o f r a b b i t s t r e a t e d w i t h t h e C-2,4-DNHPC-WD f o r m u l a t i o n were w i p e d w i t h d i s t i l l e d w a t e r o n l y . The w i p e s were e x t r a c t e d w i t h a c e t o n e and a n a l y z e d f o r t o t a l C - l a b e l . U r i n e , f e c e s , and p l a s m a were c o l l e c t e d a t i n t e r v a l s up t o 7 d a y s and a n a l y z e d f o r ^ C - l a b e l . A t t e r m i n a t i o n , t h e a p p l i c a t i o n s i t e s k i n s were c o l l e c t e d , d i s s o l v e d i n t i s s u e s o l u b i l i z e r ( U n i s o l ; I s o l a b I n c . ; A k r o n , OH), and analyzed f o r t o t a l C-label. z

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R a b b i t 7 Day ( L e a v e - O n ) Dermal E x p o s u r e S t u d y . C-2,4-DNHPC was a p p l i e d d e r m a l l y as t h e n e a t m a t e r i a l a t 25 mg/kg (2.1 mg/cm ; 30 u C i / k g ) , and was l e f t on f o r 7 d a y s . U r i n e , f e c e s , and p l a s m a were c o l l e c t e d a t i n t e r v a l s o v e r t h e 7-day p e r i o d and a n a l y z e d f o r C - l a b e l . A t t e r m i n a t i o n , . t h e a p p l i c a t i o n s i t e s k i n s were c o l l e c t e d and a n a l y z e d f o r C - l a b e l . The a p p l i c a t i o n s i t e s were not w i p e d p r i o r t o ' C - a n a l y s i s o f t h e s k i n , s i n c e a l a r g e amount o f f u r had grown b a c k . R a b b i t M u l t i p l e Dermal Dose S t u d y . Neat C-2,4-DNHPC was a p p l i e d as 13 d a i l y 6 h r d o s e s a t 25 mg/kg/day. T h e 5 x 8 cm a p p l i c a t i o n a r e a was r o t a t e d among 7 s i t e s s u c h t h a t c o n s e c u t i v e d o s e s were n o t a p p l i e d t o t h e same o r . a d j a c e n t s i t e s . The a p p l i c a t i o n s i t e s were wiped 6 hr a f t e r each C-dose a p p l i c a t i o n , and t h e w i p e s were a n a l y z e d f o r C - l a b e l . U r i n e , f e c e s , and p l a s m a were c o l l e c t e d a t i n t e r v a l s d u r i n g t h e 13 d a y d o s i n g p h a s e and f o r up t o 10 days a f t e r t h e l a s t d o s e , and a n a l y z e d f o r ' C - l a b e l . R a b b i t s were k i l l e d 10 days a f t e r t h e l a s t d o s e , and t h e a p p l i c a t i o n s i t e s were c o l l e c t e d and a n a l y z e d f o r ^ C - l a b e l . 4

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Monkey I n t r a v e n o u s S t u d y . C-2,4-DNHPC d i s s o l v e d i n DMS0, was a d m i n i s t e r e d i n t h e f e m o r a l v e i n (0.1 m l / k g ) a t 0.2 mg/kg (0.15 u C i / k g ) . P l a s m a was c o l l e c t e d a t i n t e r v a l s up t o 2 days a f t e r d o s i n g , w h i l e u r i n e and f e c e s were c o l l e c t e d a t i n t e r v a l s up t o 4 days a f t e r d o s i n g and a n a l y z e d f o r C - l a b e l . F e c a l s a m p l e s were p o o l e d p r i o r t o a n a l y s i s . T h e s e a n i m a l s were u s e d i n s u b s e q u e n t dermal s t u d i e s o n c e . i t was d e t e r m i n e d t h a t p l a s m a and u r i n e c o n ­ t a i n e d no r e s i d u a l C-label. Monkey P e r c u t a n e o u s S t u d y (40 u g / c m ) . C-2,4-DNHPC, d i s s o l v e d i n 400 u l a c e t o n e , was a p p l i e d t o 40 c m o f a b d o m i n a l s k i n a t 40 ug/cm ( 1 . 6 mg/monkey; a p p r o x i m a t e l y 0.2 mg/kg; 12 u C i / m o n k e y ) . The a n i m a l s were r e s t r a i n e d i n m e t a b o l i c c h a i r s d u r i n g t h e dermal e x p o s u r e p e r i o d , and were r e t u r n e d t o m e t a b o l i c c a g e s i m m e d i a t e l y f o l l o w i n g t h e dose wipe-off. T h e a p p l i c a t i o n s i t e s were wiped w i t h c o t t o n b a l l s l a d e n e d w i t h w a t e r , o r w i t h aqueous 9 5 % e t h a n o l f o l l o w e d by a w a t e r r i n s e 6 h r a f t e r a p p l i c a t i o n ; t h e w i p e s were 2

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Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

11. LONGACREETAL.

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a n a l y z e d f o r 1 ^ C - 1 a b e l . P l a s m a was c o l l e c t e d a t i n t e r v a l s up t o 2 d a y s , w h i l e u r i n e and f e c e s were c o l l e c t e d a t i n t e r v a l s up t o 4 days and a n a l y z e d f o r C - l a b e l . Monkey P e r c u t a n e o u s S t u d y (2500 u g / c m ) . C-2,4-DNHPC d i s s o l v e d i n 14 u l a c e t o n e , was a p p l i e d t o 0.64 cm o f a b d o m i n a l s k i n a t 2500 ug/ciTr ( 1 . 6 mg/monkey; a p p r o x i m a t e l y 0.2 mg/kg; 12 u C i / m o n k e y ) . The a p p l i c a t i o n s i t e s were w i p e d w i t h aqueous 9 5 % e t h a n o l , f o l l o w e d by w a t e r , 6 h r a f t e r dose a p p l i c a t i o n ; t h e w i p e s were a n a l y z e d f o r C - l a b e l . P l a s m a was c o l l e c t e d a t i n t e r v a l s up t o 2 d a y s , w h i l e u r i n e and f e c e s were c o l l e c t e d a t i n t e r v a l s up t o 4 days and analyzed f o r C - l a b e l . P e r c e n t A b s o r p t i o n . The f r a c t i o n o f an o r a l o r dermal dose o f i4C-2,4-DNHPC a b s o r b e d r e p r e s e n t e d t h e u r i n a r y 1 4 c - e x c r e t i o n a f t e r o r a l o r dermal a d m i n i s t r a t i o n d i v i d e d b y t h e u r i n a r y ^ C - e x c r e t i o n after i v administration (2, 3 ) . 1 4

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Results R a b b i t I n t r a v e n o u s S t u d y . Most (58-85%) o f an i v d o s e o f ' C-2,4-DNHPC was e x c r e t e d f r o m r a b b i t s w i t h i n 24-48 h r ( F i g u r e 3 ) . Urinary C - e x c r e t i o n was 5 - f o l d g r e a t e r t h a n f e c a l e x c r e t i o n ; 7 3 % o f t h e d o s e was r e c o v e r e d i n t h e u r i n e b y 96 h r . R a b b i t O r a l S t u d i e s . The p e r c e n t a b s o r p t i o n o f an o r a l dose o f 14C-2,4-DNHPC (0.5-25 mg/kg) was 60-69% { T a b l e I ) . P r a c t i c a l l y a l l o f an o r a l dose o f C-2,4-DNHPC was e l i m i n a t e d i n t h e e x c r e t a o f r a b b i t s w i t h i n 48 h r ( F i g u r e 3 ) . T h e p e r c e n t c u m u l a t i v e u r i n a r y and f e c a l C - e x c r e t i o n . w e r e each s i m i l a r among t h e t h r e e o r a l d o s e g r o u p s . F e c a l C-excretion ( 5 7 - 7 2 % o f d o s e ) was s l i g h t l y g r e a t e r t h a n u r i n a r y ^ C - e x c r e t i o n ( 3 5 - 5 1 % o f d o s e ) b y 96 h r . ' C-2,4-DNHPC-derived C - l a b e l was r a p i d l y a b s o r b e d a f t e r o r a l a d m i n i s t r a t i o n , r e a c h i n g peak p l a s m a C-concentrations within 1-3 h r ( T a b l e I I ) . Peak p l a s m a ^ - c o n c e n t r a t i o n was p r o p o r t i o n a l t o d o s e ( T a b l e I I ) . E l i m i n a t i o n o f C - l a b e l was b i p h a s i c f o r a l l g r o u p s ; a r a p i d e l i m i n a t i o n p h a s e ( t 1/2 = 2.2-3.8 h r ) , l a s t i n g a p p r o x i m a t e l y 24 h r a f t e r d o s i n g , p r e c e d e d a s l o w e r t e r m i n a l e l i m i n a t i o n p h a s e ( t 1/2 = 33.3-55.1 h r ) . +#

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R a b b i t 6 Hr Dermal E x p o s u r e S t u d i e s . The p e r c e n t a b s o r p t i o n o f a 6 h r dermal e x p o s u r e o f C-2,4-DNHPC was 4-9%, r e g a r d l e s s o f t h e dose o r t h e f o r m u l a t i o n / v e h i c l e ( T a b l e I ) . A m a j o r i t y o f t h e a p p l i e d 1 C-2,4-DNHPC ( 6 0 - 9 5 % o f d o s e ; 89-95% o f r e c o v e r e d C - l a b e l ) was r e c o v e r e d i n t h e 6 h r w i p e - o f f r e g a r d l e s s o f t h e dose o r t h e f o r m u l a t i o n / v e h i c l e ( T a b l e I I I ) . Little C - l a b e l ( 0 . 0 2 - 1 % o f d o s e ) was r e c o v e r e d i n t h e a p p l i ­ c a t i o n s i t e s k i n s a t t h e end o f t h e 7-day i n - l i f e p b a s e ( T a b l e I I I ) . A t o t a l o f 5-12% o f a 6 h r dermal e x p o s u r e o f C-2,4-DNHPC was e l i m i n a t e d i n t h e e x c r e t a w i t h i n 7 d a y s r e g a r d l e s s o f t h e dose or t h e f o r m u l a t i o n / v e h i c l e (Table I I I ) . A l s o , t h e percent c u m u l a t i v e u r i n a r y and f e c a l ' C - e x c r e t i o n were c o m p a r a b l e among t h e dermal g r o u p s , r e g a r d l e s s o f t h e d o s e o r t h e f o r m u l a t i o n / v e h i c l e . Most o f t h e e x c r e t e d C - l a b e l was e l i m i n a t e d w i t h i n 2-4 days ( F i g u r e 3 ) , and was e s s e n t i a l l y e v e n l y d i s t r i b u t e d between t h e u r i n e and f e c e s . 14

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Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

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P e r c e n t A b s o r p t i o n o f C-2,4-DNHPC i n Female R a b b i t s and Rhesus Monkeys

Route

Exposure Time

Formulation/ Vehicle

Percent Absorption

Rabbit

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3 0.5 3 25

— — — —

3

iv

4 3 4

Oral Oral Oral

— — — —

Gum T r a g Gum T r a g Gum T r a g

3 1 2

Neat

13 +

6

Neat

6 +

1

Dermal Dermal Dermal

6 Hr 6 Hr 6 Hr

25 25 25

2390 2450 2220

3 3 4

Dermal Dermal Dermal

6 Hr 6 Hr 6 Hr

25

2060

4

Dermal

4

Dermal

4

iv



DMSO

7 Day

69 + 29 60 + 4 64 + 6

9 + 4 + 7 +

3 3 3

6 Hr ( x l 3 )

6

2 3 4

2150 8310 18,300

1850-2313

b

4 + 5 + 5 +

25 100 220

25

100 +

DMSO

Neat Neat Neat WD LC Acetone

Monkey 0.2



100 + 16

0.2

40

8

Dermal

6 Hr

Acetone

16 +

7

0.2

2500

4

Dermal

6 Hr

Acetone

5 +

3

P e r c e n t a b s o r p t i o n (% o f d o s e ) ; mean + s t a n d a r d d e v i a t i o n . One

(1) p e r c e n t gum t r a g a c a n t h

suspension.

F i g u r e 3. C u m u l a t i v e e x c r e t i o n o f C - l a b e l i n t h e u r i n e ( O h f e c e s ( • ) , and combined u r i n e and f e c e s ( • ) o f f e m a l e r a b b i t s a d m i n i s t e r e d a n ^ v , o r a l , 6 h r d e r m a l , o r 7-day ( l e a v e - o n ) dermal dose o f C-2,4-DNHPC.

Wang et al.; Biological Monitoring for Pesticide Exposure ACS Symposium Series; American Chemical Society: Washington, DC, 1988.

a

11. LONGACRE ET AL.

143

Dinocap Dermal Absorption

1 4

Table I I .

Peak P l a s m a C - C o n c e n t r a t i o n i n Female R a b b i t s and Rhesus Monkeys A d m i n i s t e r e d C-2,4-DNHPC

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14

Dose mg/kg u g / c m

2

Exposure Route Time

Formulation/ Vehicle n

1 4

Peak P l a s m a C-Concentration (ppm) (hr)

Rabbit

— — —

0. 5 3 25

Oral Oral Oral

— — —

Gum Gum Gum

Trag Trag Trag

4 3 4

0.29 + 0.04 1.26 + 0.42 14.55 + 6.62

1 3 3

3 3 3

0.15 + 0.05 0.47 + 0.10 1.51 + 1.12

6 24

3 3 4

0.19 + 0.03 0.24 + 0.07 0.28 + 0.00

24 6 24

25 100 220

2150 8310 18i,300

Dermal Dermal Dermal

6 Hr 6 Hr 6 Hr

25 25 25

2390 2450 2220

Dermal Dermal Dermal

6 Hr 6 Hr 6 Hr

25

2060

Dermal

7 Day

Neat

4

0.24 + 0.19

6

18502313

Dermal

6 Hr (xl3)

Neat

4

0.89

+ 0.33

318

25 (X13)

Neat Neat Neat

b

WD LC Acetone

Monkey

a

0