Protein Tyrosine Phosphatase 1B Inhibitors: A Molecular Level Legitimate Approach for the Management of Diabetes Mellitus

Thareja, Suresh; Aggarwal, Saurabh; Bhardwaj, T. R.; Kumar, Manoj

doi:10.1002/med.20219

Cited by 109 publications

(71 citation statements)

References 189 publications

(195 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…100,101 In mice, genetic ablation of protein tyrosine phosphatase 1B (PTP-1B) results in enhanced insulin sensitivity. 102 ISI-113175 (ISIS Pharmaceuticals), an antisense oligonucleotide PTP-1B inhibitor (100-200 mg injected weekly), has completed a phase 2 trial in patients with type 2 diabetes on stable, maximal doses of SU.…”

Section: 99mentioning

confidence: 99%

Novel Agents for the Treatment of Type 2 Diabetes

DeFronzo¹,

Triplitt²,

Abdul‐Ghani³

et al. 2014

Diabetes Spectrum

View full text Add to dashboard Cite

In Brief Impaired insulin secretion, increased hepatic glucose production, and decreased peripheral glucose utilization are the core defects responsible for the development and progression of type 2 diabetes. However, the pathophysiology of this disease also includes adipocyte insulin resistance (increased lipolysis), reduced incretin secretion/sensitivity, increased glucagon secretion, enhanced renal glucose reabsorption, and brain insulin resistance/neurotransmitter dysfunction. Although current diabetes management focuses on lowering blood glucose, the goal of therapy should be to delay disease progression and eventual treatment failure. Recent innovative treatment approaches target the multiple pathophysiological defects present in type 2 diabetes. Optimal management should include early initiation of combination therapy using multiple drugs with different mechanisms of action. This review examines novel therapeutic options that hold particular promise.

show abstract

Section: 99mentioning

confidence: 99%

Novel Agents for the Treatment of Type 2 Diabetes

DeFronzo¹,

Triplitt²,

Abdul‐Ghani³

et al. 2014

Diabetes Spectrum

View full text Add to dashboard Cite

show abstract

“…Способность ингибиро-вания цитоплазматической фосфатазы PTP1B явля-ется основанием и перспективным направлением поиска новых лекарственных средств для лечения СД2. Однако большинство исследований в данном направлении ведется на уровне молекулярного кон-струирования и синтеза высокоселективных, до-ступных для перорального приема ингибиторов, и анализа зависимости между химической структу-рой, физико-химическими свойствами и функцио-нальной активностью полученных соединений [56].…”

Section: активация и потенцирование инсулиновой сигна-лизации улучшеunclassified

Promising pharmacological targets for the treatment of the diseases associated with the impaired insulin receptor signaling pathway

Gorbunov

Brigadirova

Качаева

et al. 2015

Probl Endokrinol (Mosk)

View full text Add to dashboard Cite

ОБЗОРЫСахарный диабет (СД) занимает одно из первых мест в мире среди наиболее распространенных хро-нических заболеваний. В ряд социально значимых заболеваний СД ставят такие его особенности, как большая частота встречаемости, высокий риск ин-валидизации и смертности больных. В 2013 г., по данным Международной диабетической федерации, численность больных СД в мире составила 386 млн человек. Учитывая темпы распространения заболе-вания, согласно прогнозам экспертов ВОЗ, число пациентов с диагнозом СД достигнет к 2035 г. 592 млн человек в основном за счет больных СД 2-го типа (СД2) [1]. По данным Минздрава России, уро-вень инвалидизации по причине СД составляет 2,1 случая на 100 тыс. населения [2].СД представляет собой гетерогенную группу ме-таболических расстройств, которые характеризуют-ся общим симптомом -хронической гиперглике-мией, а также абсолютным или относительным де-фицитом продукции инсулина, либо его действия [3]. СД 1-го типа возникает из-за недостаточной продукции инсулина вследствие потери функцио- Diabetes mellitus (DM) is one of the most widespread chronic diseases in the world. In DM type 2, peripheral tissues demonstrate strong resistance to endogenous insulin (insulin resistance) which is caused by impaired ability of the hormone to stimulate glucose uptake in target cells (muscle, adipose or brain tissue, liver, etc.) and to reduce blood glucose level. Research data suggest that all mentioned reasons are most likely to be based on a disruption of signal transduction from insulin receptor (IR) into insulin-dependent intracellular signaling cascades. Contemporary DM treatment strategy is aimed at the maintenance of optimal blood glucose level by improving insulin production and increasing insulin sensitivity of tissue as well as prevention of macro-and microvascular complications and decrease of their intensity. At the same time, the search for new targets for creation of innovative anti-diabetic compounds can be considered a promising task due to the optimization of existing approaches and development of the novel ones taking into account results of the latest research into DM etiology and pathogenesis. A special position among possible targets is occupied by insulin receptor (IR) and IR-associated signaling pathways. Belonging to tyrosine kinase receptor family, IR has been actively studied during the last decades. This review considers in particular the IR structure and functioning of receptor-associated signaling pathways. The paper contains data on novel ligand-mimetics and IR sensitizers as well as other molecules, which affect different components of IR-associated signaling pathways, thus exerting significant antidiabetic effect. Action of these compounds is aimed at improvement of basic metabolic disorders resulting in hyperglycemia and is mainly carried out due to the following effects: activation and potentiation of insulin signaling, increase of insulin sensitivity of peripheral tissues; recovery of insulin secretion physiological mechanisms; reduction of glucose production in liver.

show abstract

“…Several experiments have also demonstrated that the knockout of PTP1B in mice can result in insulin hypersensitivity, even in a high-fat diet. [1][2][3][4][5][6] Therefore; small molecular inhibitors of PTP1B are promising drugs for curing type II diabetes. The full length of PTP1B consists of 435 amino acids, constituting the major cellular form; however, only a shorter length of 298 or 321 residues is typically considered in biochemical studies.…”

Section: Introductionmentioning

confidence: 99%

The Molecular Modeling of Novel Inhibitors of Protein Tyrosine Phosphatase 1B Based on Catechol by MD and MM-GB (PB)/SA Calculations

Kocakaya¹

2014

Bulletin of the Korean Chemical Society

View full text Add to dashboard Cite

Binding modes of a series of catechol derivatives such as protein tyrosine phosphatase 1B (PTP1B) inhibitors were identified by molecular modeling techniques. Docking, molecular dynamics simulations and free energy calculations were employed to determine the modes of these new inhibitors. Binding free energies were calculated by involving different energy components using the Molecular Mechanics-Poisson-Boltzmann Surface Area and Generalized Born Surface Area methods. Relatively larger binding energies were obtained for the catechol derivatives compared to one of the PTP1B inhibitors already in use. The Molecular Mechanics/ Generalized Born Surface Area (MM/GBSA) free energy decomposition analysis indicated that the hydroxyl functional groups and biphenyl ring system had favorable interactions with Met258, Tyr46, Gln262 and Phe182 residues of PTP1B. The results of hydrogen bound analysis indicated that catechol derivatives, in addition to hydrogen bonding interactions, Val49, Ile219, Gln266, Asp181 and amino acid residues of PTP1B are responsible for governing the inhibitor potency of the compounds. The information generated from the present study should be useful for the design of more potent PTP1B inhibitors as anti-diabetic agents.

show abstract

Protein Tyrosine Phosphatase 1B Inhibitors: A Molecular Level Legitimate Approach for the Management of Diabetes Mellitus

Cited by 109 publications

References 189 publications

Novel Agents for the Treatment of Type 2 Diabetes

Novel Agents for the Treatment of Type 2 Diabetes

Promising pharmacological targets for the treatment of the diseases associated with the impaired insulin receptor signaling pathway

The Molecular Modeling of Novel Inhibitors of Protein Tyrosine Phosphatase 1B Based on Catechol by MD and MM-GB (PB)/SA Calculations

Contact Info

Product

Resources

About