Taurine-Derived Compounds Produce Anxiolytic Effects in Rats Following Developmental Lead Exposure

Lorenz S Neuwirth; Bright U Emenike; George B Cruz; Ericka Cabañas; Michelle A Vasquez; Jewel N Joseph; Zaid Ayaz; Mohammed Mian; Mohamed M Ali; Evan G Clarke; Eddy D Barrera; Nimra Hameed; Samantha Rubi; Teddy F Dacius Jr; Jourvonn C Skeen; Jalen R Bonitto; Eric B Khairi; Asma Iqbal; Isra Ahmed; Tokunbo J Jose; Kirsten P Lynch; Amber Alivira; Neena Mathew; Sukhpreet Kaur; Sidrah Masood; Bettina Tranquilee; Veni Thiruverkadu

doi:10.1007/978-3-030-93337-1_42

Taurine-Derived Compounds Produce Anxiolytic Effects in Rats Following Developmental Lead Exposure

Adv Exp Med Biol. 2022:1370:445-460. doi: 10.1007/978-3-030-93337-1_42.

Authors

Lorenz S Neuwirth^{1

2}, Bright U Emenike³, George B Cruz^{4

5}, Ericka Cabañas^{4

5}, Michelle A Vasquez^{4

3}, Jewel N Joseph^{4

5}, Zaid Ayaz^{4

5}, Mohammed Mian^{4

5}, Mohamed M Ali^{4

5}, Evan G Clarke^{4

5}, Eddy D Barrera^{6

4}, Nimra Hameed^{4

5}, Samantha Rubi^{4

5}, Teddy F Dacius Jr^{6

4}, Jourvonn C Skeen^{4

5}, Jalen R Bonitto^{4

5}, Eric B Khairi^{4

5}, Asma Iqbal^{6

4}, Isra Ahmed^{6

4}, Tokunbo J Jose^{6

4}, Kirsten P Lynch^{6

4}, Amber Alivira^{6

4}, Neena Mathew^{6

4}, Sukhpreet Kaur^{6

4}, Sidrah Masood^{6

4}, Bettina Tranquilee^{4

5}, Veni Thiruverkadu^{4

5}

Affiliations

¹ Department of Psychology, SUNY Old Westbury, Old Westbury, NY, USA. neuwirthl@oldwestbury.edu.
² SUNY Neuroscience Research Institute, SUNY Old Westbury, Old Westbury, NY, USA. neuwirthl@oldwestbury.edu.
³ Department of Chemistry and Physics, SUNY Old Westbury, Old Westbury, NY, USA.
⁴ SUNY Neuroscience Research Institute, SUNY Old Westbury, Old Westbury, NY, USA.
⁵ Department of Biology, SUNY Old Westbury, Old Westbury, NY, USA.
⁶ Department of Psychology, SUNY Old Westbury, Old Westbury, NY, USA.

PMID: 35882818
DOI: 10.1007/978-3-030-93337-1_42

Abstract

Lead (Pb²⁺) is a developmental neurotoxicant that disrupts the GABA-shift and subsequently causes alterations in the brain's excitation-to-inhibition (E/I) balance. Taurine is a well-established neuroprotective and inhibitory compound for regulating brain excitability. Since mechanistically taurine can facilitate neuronal inhibition through the GABA-_AR, the present study examined the anxiolytic potential of taurine derivatives. Treatment groups consisted of the following developmental Pb²⁺-exposures: Control (0 ppm) and Perinatal (150 ppm or 1,000 ppm lead acetate in the drinking water). Rats were scheduled for behavioral tests between postnatal days (PND) 36-45 with random drug assignments to either saline, taurine, or taurine-derived compound (TD-101, TD-102, or TD-103) to assess the rats' responsivity to each drug in mitigating the developmental Pb²⁺-exposure and anxiety-like behaviors through the GABAergic system. Long-Evans hooded rats were assessed using an open field (OF) test for preliminary locomotor assessment. Twenty-four hours later, the same rats were exposed to the elevated plus maze (EPM) and were given an i.p. injection of 43 mg/Kg of the saline, taurine, or TD drugs 15 min prior to testing. Each rat was tested using the triple-blind random assignment method for each drug condition. The OF data revealed that Control female rats had increased locomotor activity over Control male rats, and the Pb²⁺-exposed males and females had increased locomotor activity when compared to the Control male and female rats. However, in the EPM, the Control female rats exhibited more anxiety-like behaviors over Control male rats, and the Pb²⁺-exposed male and female rats showed selective responsivity to TD drugs when compared to taurine. For Pb²⁺-exposed males, TD-101 showed consistent recovery of anxiety-like behaviors similar to that of taurine regardless of Pb²⁺ dose, whereas in Pb²⁺-exposed females TD-101 and TD-103 showed greater anxiolytic responses in the EPM. The results from the present psychopharmacological study suggests that taurine and its derivatives are interesting drug candidates to explore sex-specific mechanisms and actions of taurine and the associated GABAergic receptor properties by which these compounds alleviate anxiety as a potential behavioral pharmacotherapy for neurodevelopmental Pb²⁺ exposure.

Keywords: Anxiety-like behaviors; Anxiolytic drugs; Developmental lead (Pb2+) exposure; GABAergic system; Lead poisoning; Taurine derivatives.

MeSH terms

Animals
Anti-Anxiety Agents* / pharmacology
Anti-Anxiety Agents* / therapeutic use
Anxiety / chemically induced
Anxiety / drug therapy
Female
Lead / toxicity
Male
Pregnancy
Rats
Rats, Long-Evans
Taurine / pharmacology
Taurine / therapeutic use
gamma-Aminobutyric Acid

Substances

Anti-Anxiety Agents
gamma-Aminobutyric Acid
Lead
Taurine