Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma

Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma

Integrin αvβ3 receptors are overexpressed in different tumors and their associated neovascularization and hence, represent a potential cancer target. We previously synthesized a high affinity thyrointegrin αvβ3, P<sub>4000</sub>-bi-TAT (tetrac derivative), with potent anticancer properti...

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Main Authors: Kavitha Godugu, Mehdi Rajabi, Shaker A. Mousa
Format: Article
Language:English
Published: MDPI AG 2021-06-01
Series:Cancers
Subjects:
anticancer
glioblastoma
anti-angiogenesis
thyrointegrin αvβ3
PEG
triazole tetrac
Online Access:https://www.mdpi.com/2072-6694/13/11/2780
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spelling doaj-3e01518412f04d44bfe9947e19faad0e2021-06-30T23:12:11ZengMDPI AGCancers2072-66942021-06-01132780278010.3390/cancers13112780Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in GlioblastomaKavitha Godugu0Mehdi Rajabi1Shaker A. Mousa2The Pharmaceutical Research Institute, Albany College of Pharmacy and Health Sciences, Rensselaer, NY 12208, USAThe Pharmaceutical Research Institute, Albany College of Pharmacy and Health Sciences, Rensselaer, NY 12208, USAThe Pharmaceutical Research Institute, Albany College of Pharmacy and Health Sciences, Rensselaer, NY 12208, USAIntegrin αvβ3 receptors are overexpressed in different tumors and their associated neovascularization and hence, represent a potential cancer target. We previously synthesized a high affinity thyrointegrin αvβ3, P<sub>4000</sub>-bi-TAT (tetrac derivative), with potent anticancer properties. However, the long polydisperse PEG conjugate showed large scaleup and analytical/bioanalytical issues. Hence, in the present study, we synthesized a mono versus bi-triazole tetrac with discrete monodisperse PEG, which provided improvement in scaleup and bioanalysis. In the present study, we compared binding affinity and anticancer activates with a smaller PEG size (P<sub>1600</sub>-bi-TAT, Compound <b>2</b>) and the removal of one TAT molecule (P<sub>1600</sub>-m-TAT, Compound <b>3</b>) versus P<sub>4000</sub>-bi-TAT, Compound <b>1</b>. The results of the selectivity and affinity of TATs showed greater affinity to integrin αvβ3. The xenograft weights and tumor cell viabilities were decreased by >90% at all doses compared to the control (ON Treatment, *** <i>p</i> < 0.001) in cells treated with Compounds <b>1</b>, <b>2</b>, and <b>3</b> in U87-Luc-treated mice. The in vivo luminescent signals of U87-luc cells reflect the proliferation and distribution of tumor cells in the animals and the maximum intensity corresponding to the maximum tumor cells that the animals could tolerate. We found that the three thyrointegrin αvβ3 antagonists exhibited optimal therapeutic efficacy against U87 or primary glioblastoma cells. Biological studies showed that decreasing the PEG linker size (1600 vs. 4000) or having mono-TAT or bi-TAT had no significant impact on their αvβ3 binding affinity, anti-angiogenesis, or overall anti-cancer efficacy.https://www.mdpi.com/2072-6694/13/11/2780anticancerglioblastomaanti-angiogenesisthyrointegrin αvβ3PEGtriazole tetrac
collection DOAJ
language English
format Article
sources DOAJ
author Kavitha Godugu
Mehdi Rajabi
Shaker A. Mousa
spellingShingle Kavitha Godugu
Mehdi Rajabi
Shaker A. Mousa
Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
Cancers
anticancer
glioblastoma
anti-angiogenesis
thyrointegrin αvβ3
PEG
triazole tetrac
author_facet Kavitha Godugu
Mehdi Rajabi
Shaker A. Mousa
author_sort Kavitha Godugu
title Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
title_short Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
title_full Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
title_fullStr Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
title_full_unstemmed Anti-Cancer Activities of Thyrointegrin α<sub>v</sub>β<sub>3</sub> Antagonist Mono- and Bis-Triazole Tetraiodothyroacetic Acid Conjugated via Polyethylene Glycols in Glioblastoma
title_sort anti-cancer activities of thyrointegrin α<sub>v</sub>β<sub>3</sub> antagonist mono- and bis-triazole tetraiodothyroacetic acid conjugated via polyethylene glycols in glioblastoma
publisher MDPI AG
series Cancers
issn 2072-6694
publishDate 2021-06-01
description Integrin αvβ3 receptors are overexpressed in different tumors and their associated neovascularization and hence, represent a potential cancer target. We previously synthesized a high affinity thyrointegrin αvβ3, P<sub>4000</sub>-bi-TAT (tetrac derivative), with potent anticancer properties. However, the long polydisperse PEG conjugate showed large scaleup and analytical/bioanalytical issues. Hence, in the present study, we synthesized a mono versus bi-triazole tetrac with discrete monodisperse PEG, which provided improvement in scaleup and bioanalysis. In the present study, we compared binding affinity and anticancer activates with a smaller PEG size (P<sub>1600</sub>-bi-TAT, Compound <b>2</b>) and the removal of one TAT molecule (P<sub>1600</sub>-m-TAT, Compound <b>3</b>) versus P<sub>4000</sub>-bi-TAT, Compound <b>1</b>. The results of the selectivity and affinity of TATs showed greater affinity to integrin αvβ3. The xenograft weights and tumor cell viabilities were decreased by >90% at all doses compared to the control (ON Treatment, *** <i>p</i> < 0.001) in cells treated with Compounds <b>1</b>, <b>2</b>, and <b>3</b> in U87-Luc-treated mice. The in vivo luminescent signals of U87-luc cells reflect the proliferation and distribution of tumor cells in the animals and the maximum intensity corresponding to the maximum tumor cells that the animals could tolerate. We found that the three thyrointegrin αvβ3 antagonists exhibited optimal therapeutic efficacy against U87 or primary glioblastoma cells. Biological studies showed that decreasing the PEG linker size (1600 vs. 4000) or having mono-TAT or bi-TAT had no significant impact on their αvβ3 binding affinity, anti-angiogenesis, or overall anti-cancer efficacy.
topic anticancer
glioblastoma
anti-angiogenesis
thyrointegrin αvβ3
PEG
triazole tetrac
url https://www.mdpi.com/2072-6694/13/11/2780
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AT mehdirajabi anticanceractivitiesofthyrointegrinasubvsubbsub3subantagonistmonoandbistriazoletetraiodothyroaceticacidconjugatedviapolyethyleneglycolsinglioblastoma
AT shakeramousa anticanceractivitiesofthyrointegrinasubvsubbsub3subantagonistmonoandbistriazoletetraiodothyroaceticacidconjugatedviapolyethyleneglycolsinglioblastoma
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