Е. М. Трещалина scite author profile

Е. М. Трещалина

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Pathological Metabolism of Methionine in Malignant Cells Is a Potential Target for the Antitumor Therapy

VS¹,

Davydov²,

Anufrieva³

et al. 2017

Клиническая онкогематология

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This review presents the characteristics of the cellular metabolism of methionine, as well as known data on the mechanisms of the development of methionine dependence in malignant cells. The possibilities of using a non-methionine diet for the control of the tumor growth in patients with various forms of cancer are considered. The information about methionine Y-lyase, an enzyme providing elimination of methionine from plasma, is provided. Its role as a potential antitumor enzyme is disclosed. Data on cytotoxic activity of the enzyme, obtained from various sources, and information on tumor models and cell cultures, showing methionine dependence are summarised.

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Use of Pyridoxine to Increase Anticacner Activity of Methionine-Gamma-Lyase in Murine Cancer Models

Davydov¹,

Морозова²,

Комарова

et al. 2017

Sib. onkol. ž.

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Приведены экспериментальные данные монотерапии и комбинированной терапии моделей перевиваемых опухолей мышей препаратами метионин-γ-лиазы (МГЛ) и пиридоксина гидрохлорида. Изучены МГЛ Clostridium sporogenes и Citrobacter freundii. Использованы перевиваемые модели опухолей мышей: карцинома легкого Льюис (LLC), меланома В16, лимфолейкоз P388, лимфолейкоз L1210, лимфаденоз Фишера L5178y. На моделях P388, L5178y МГЛ не показала противоопухолевой активности ни в монорежиме, ни в сочетании с пиридоксином. На модели L1210 было получено пограничное увеличение продолжительности жизни (УПЖ) 22 %, р=0,035 при применении МГЛ C. sporogenes в дозе 2000 Е/кг 11-кратно внутрибрюшинно с интервалом 12 ч. На LLC показано, что на 1-е сут после окончания лечения одновременное внутрибрюшное (в/б) введение МГЛ C. sporogenes 400 Е/кг 4-кратно с интервалом 48 ч и пиридоксина в дозе 250 мг/кг вызывало ТРО=55 % (р<0,001), монотерапия МГЛ или пиридоксином в аналогичных дозах и режимах применения вызывала ТРО=24 % (р=0,263) и 21 % (р=0,410) соответственно. При попарном сравнении: комбинированная терапия МГЛ + пиридоксин против монотерапии МГЛ в аналогичном режиме р=0,061, против монотерапии пиридоксином р=0,031. На LLC МГЛ C. freundii 200 Е/кг 4-кратно с интервалом 48 ч и пиридоксина в дозе 500 мг/кг одновременно на 9-е сут после окончания лечения вызывало ТРО=50 % (р=0,001), при этом монотерапия МГЛ в разовой дозе 400 Е/кг или пиридоксином в аналогичном режиме применения вызывала ТРО=+5 % (р=0,991) и 4 % (р=0,998) соответственно. При попарном сравнении: комбинированная терапия МГЛ 200 Е/кг + пиридоксин против монотерапии МГЛ 400 Е/кг в аналогичном режиме р<0,001, против монотерапии пиридоксином р=0,003. На модели меланома B16 МГЛ 2000 в/б + пиридоксин 300 мг/кг вызывает ТРО 56 % на 1-е сут (р=0,045) и 35 % на 3-и сут (р=0,038). При комбинированной терапии МГЛ + пиридоксин последний значимо повышал противоопухолевую активность МГЛ в сочетаниях: МГЛ 1000 Е/кг в/б и МГЛ 1000 Е/кг в/б + пиридоксин 300 мг/кг ТРО=45 % (р=0,034) на 3-и сут после окончания лечения. При внутривенном введении МГЛ 500 Е/кг и МГЛ 500 Е/кг + пиридоксин последний повышал эффективность лечения: максимальное ТРО 50 % на 1-е сут после окончания лечения (р=0,085, различие не достоверно) и 21 % на 3-и сут после окончания лечения ТРО 22 % (р=0,965, различие не достоверно).

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Ribonucleases with Antiproliferative Properties: Molecular Biological and Biochemical Characteristics

Покровский¹,

Трещалина²,

Nv³

et al. 2016

Клиническая онкогематология

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The article dwells on ribonucleases (RNAses) whose cytotoxic activity depends on the enzymatic activity, i.e. the ability to catalyze the cleavage of phosphodiester bonds of RNA. It presents both well-known information and our own data on RNAses of different origins with antitumor properties; it investigates the relation between the mechanism of cytotoxicity and biochemical and molecular biological characteristics. The analysis of published data demonstrates that all above characteristics contribute to the antiproliferative activity of RNAses. The major challenge for this group of enzymes is the achieving of selective bioavailability. This problem can be solved by creating conjugates as in case with ranpirnase and barnase. Based on their major pharmacological properties, active antitumor RNAses have great perspectives for treatment of not only oncohematological, but also solid malignancies.

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Phyto-anti-estrogens are potential selective modifiers of biological reactions in breast cancer

Borisova¹,

Smirnova²,

Шубина³

et al. 2016

Russ. J. Onco.

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The review analyzes up-to-date information about specific characteristics of anti-estrogen therapeutic agents with different mechanisms of action with regard to present knowledge of endocrine therapy for estrogen-positive breast cancer (ER+ BC). The paper presents some agents for anti-estrogen therapy of breast cancer - aromatase inhibitors and selective modifiers of biological reactions (SMBR) and their mechanisms of anti-proliferative action. The authors describe significant therapeutic and side effects as well as different options for anti-estrogen combinations. Special emphasis is made on national herbal estrogens/anti-estrogens that have no toxicity associated with the well-known SMBRs. The review presents the structure and characteristics of a perspective phyto-anti-estrogen sekoizolaricirezinol (SEKO), which demonstrated significant anti-proliferative activity with no pro-estrogen action in the in vivo models of ER+ BC.

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