Novija istraživanja ukazuju da svaka izloženost olovu, pa čak i veoma niskim dozama može
biti štetna. Podaci o toksičnim mehanizmima i efektima olova iz dosadašnjih animalnih i humanih
studija se uglavnom zasnivaju na izloženosti visokim dozama, te stoga postoji potreba da se ispitaju
mehanizmi toksičnog dejstva i da se utvrde toksični efekti u uslovima produžene izloženosti niskim
dozama olova. Imajući navedeno u vidu, cilj ove disertacije bio je da se na modelu subakutne
izloženosti pacova ispita uticaj niskih doza olova na različite organe i sisteme organa.
Studija je sprovedena na animalnom modelu Wistar pacova koji su podeljeni u 7 grupa po 6
jedinki od kojih je jedna grupa bila kontrolna a 6 ostalih grupa je tretirano tokom 28 dana rastućim
dozama olova 0,1; 0,5; 1; 3; 7; 15 mg Pb/kg t.m./dan. Nakon 24 h od poslednje doze, pacovi su
žrtvovani na human način a krv i organi su uzeti na dalju analizu. U krvi su određivani hematološki
parametri, biohemijski parametri, hormoni, parame...tri oksidativnog statusa, bioelementi i olovo, dok
su organi podvrgnti patohistološkoj analizi i u njima su određivani parametri oksidativnos stausa,
bioelementi, olovo i aktivnost enzima acetilholinesteraze. Primena olova u šest niskih rastućih doza
omogućila je modelovanje odnosa doza-odgovor i dobijanje Benchmark doza za ispitivane toksične
efekte.
Rezultati su pokazali da olovo pri niskim dozama, može ispoljiti toksične efekte skoro na svim
ispitivanim organima. Dobijeni rezultati daju uvid u distribuciju olova između krvi i tkiva kao i
internim dozama olova koje dovode do štetnih efekata. Izmenjeni profil hematoloških i biohemijskih
parametara, zajedno sa izmenjenim nivoima bioelemenata, nastalim oksidativnim stresom,
izmenjenom aktivnošću acetilholinesteraze i patohistološkom analizom ispitivanih tkiva, ukazuju na
toksične efekte nakon subakutne oralne ekspozicije olovu. Najveći naučni doprinos ove doktorske
disertacije je ispitivanje zavisnosti doza–odgovor za svaki pojedinačni parametar kao i određivanje
Benchmark doze, koja će dalje doprineti sigurnijoj proceni rizika po zdravlje ljudi pri izloženosti
niskim dozama olova. Najniža Benchmark doza dobijena u studiji je za efekat smanjenja nivoa
testosterona u serumu pacova što predstavlja kritični toksični efekat studije. Sledeći efekti jesu
inhibicija SOD u bubrezima, povećanje nivoa Cu u femuru, sniženje Cu u krvi i povećanje MDA u
srcu, a zatim, povećanje TOS u mozgu, povećanje Zn u pankreasu i sniženje Cu u jetri.
Recent research indicates that exposure to very low lead doses can be harmful. Data on the
toxic mechanisms and effects of lead from previous animal and human studies are mainly based on
exposure to high doses, and therefore there is a need to investigate the toxic mechanism and to
determine toxic effects under conditions of prolonged exposure to low lead doses. Having this in
mind, the aim of this dissertation was to examine the effects of low lead doses on various organs and
organ systems in a subacute exposure rat model.
The study was conducted on an animal model of Wistar rat. The rats were divided into 7
groups, with 6 rats in each, where one of the them was a control group. The rats from 6 other groups
were treated for 28 days with increasing doses of 0.1; 0.5; 1; 3; 7; 15 mg Pb /kg b.w./day. After 24
hours from the last dose, rats were sacrificed and blood and organs were taken away for further
analysis. Haematological parameters, biochemical parameters, hormones, oxidative stat...us
parameters, bioelements, and lead were determined in the blood, while the organs were subjected to
pathohistological analysis and determination of oxidative status parameters, bioelements, lead and
acetylcholinesterase enzyme activity. The use of lead in six low-increasing doses enable the
modelling of the dose-response relationship and the obtaining of the Benchmark dose for the tested
toxic effects.
The results showed that lead at low doses can have toxic effects on almost all examined
organs. The obtained results provide insight into the distribution of the lead between blood and tissues
as well as the internal doses of lead that lead to harmful effects. Altered profiles of hematological and
biochemical parameters, together with altered levels of bioelements, oxidative stress, altered
acetylcholinesterase activity, and pathohistological analysis of examined tissues, indicate adverse
effects after subacute lead exposure. The greatest scientific contribution of this doctoral dissertation
is the examination of dose-response relationships for each individual parameter as well as the
determination of the Benchmark dose, which will further contribute to a safer assessment of human
health risk of low lead dose exposure. The lowest Benchmark dose obtained in the study was for the
effect of reducing testosterone levels in rat serum, which is a critical toxic effect of the study. The
next determined effects are inhibition of SOD in the kidneys, increased levels of Cu in the femur,
decreased Cu in the blood and increased MDA levels in the heart, then, an increase in TOS in the
brain, an increase in Zn in the pancreas and a decrease in Cu in the liver.
