Association between mitochondrial DNA 4,977 bp deletion and NAD(P)H:quinone oxidoreductase 1 C609T polymorphism in human breast tissues

Tseng, Ling Ming; Yin, Pen Hui; Tsai, Yi Fang; Wen, Chin; Wu, Chew Wun; Lee, Liang Ming

doi:10.3892/or_00000337

Cited by 9 publications

(2 citation statements)

References 24 publications

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“…Various carcinoma cells exhibit large-scale mtDNA deletion, such as 4977 bp, which inhibit the reduction of 5 tRNA genes and 7 protein-encoding genes. NADPH quinone oxidoreductase 1 (NQO1) deficiency enhances the ROS production in oral and breast cancer due to mtDNA 4977 gene deletion [ 57 – 60 ]. The mtDNA mutations affect the complex I of the electron transport chain in metastatic cancers.…”

Section: Introductionmentioning

confidence: 99%

Mitochondrial dysfunction, UPRmt signaling, and targeted therapy in metastasis tumor

Keerthiga

Pei

2021

Cell Biosci

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In modern research, mitochondria are considered a more crucial energy plant in cells. Mitochondrial dysfunction, including mitochondrial DNA (mtDNA) mutation and denatured protein accumulation, is a common feature of tumors. The dysfunctional mitochondria reprogram molecular metabolism and allow tumor cells to proliferate in the hostile microenvironment. One of the crucial signaling pathways of the mitochondrial dysfunction activation in the tumor cells is the retrograde signaling of mitochondria-nucleus interaction, mitochondrial unfolded protein response (UPRmt), which is initiated by accumulation of denatured protein and excess ROS production. In the process of UPRmt, various components are activitated to enhance the mitochondria-nucleus retrograde signaling to promote carcinoma progression, including hypoxia-inducible factor (HIF), activating transcription factor ATF-4, ATF-5, CHOP, AKT, AMPK. The retrograde signaling molecules of overexpression ATF-5, SIRT3, CREB, SOD1, SOD2, early growth response protein 1 (EGR1), ATF2, CCAAT/enhancer-binding protein-d, and CHOP also involved in the process. Targeted blockage of the UPRmt pathway could obviously inhibit tumor proliferation and metastasis. This review indicates the UPRmt pathways and its crucial role in targeted therapy of metastasis tumors.

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Section: Introductionmentioning

confidence: 99%

Mitochondrial dysfunction, UPRmt signaling, and targeted therapy in metastasis tumor

Keerthiga

Pei

2021

Cell Biosci

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“…A enzima quinona óxido-redutase (NOQ1) é membro da família NAD(P)Hdehidrogenase e é amplamente expressa na fase II de detoxificação. Envolvida no metabolismo das quinonas, a enzima NAD(P)H: quinona oxidorredutase 1 (NQO1) é uma redutase obrigatória de dois elétrons que participa, predominantmente, da proteção contra efeitos tóxicos de quimioterápicos e na defesa contra ROS (Nioi e Hayes, 2004;Tseng LM et al, 2009).…”

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A influência dos polimorfismos CYP1A1 A4889G, CYP1A1 T6235C, NQO1 C609T e GSTP1 Ile105Val e da deleção homozigótica de GSTM1 e GSTT1 no risco e prognóstico dos pacientes com linfoma não-Hodgkin difuso de grandes células B

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A influência dos polimorfismos CYP1A1 A4889G, CYP1A1 T6235C, NQO1 C609T e GSTP1 Ile105Val e da deleção homozigótica dos genes GSTM1 e GSTT1 no risco e prognóstico dos pacientes com linfoma não-Hodgkin difuso de grandes células B Campinas 2016 MÁRCIA TORRESAN DELAMAIN A influência dos polimorfismos CYP1A1 A4889G, CYP1A1 T6235C, NQO1 C609T e GSTP1Ile105Val e da deleção homozigótica dos genes GSTM1 e GSTT1 no risco e prognóstico dos pacientes com linfoma não-Hodgkin difuso de grandes células B

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Roles of dioxins and heavy metals in cancer and neurological diseases using ROS-mediated mechanisms

Matés

Segura

Alonso

et al. 2010

Free Radical Biology and Medicine

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112

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Association between mitochondrial DNA 4,977 bp deletion and NAD(P)H:quinone oxidoreductase 1 C609T polymorphism in human breast tissues

Cited by 9 publications

References 24 publications

Mitochondrial dysfunction, UPRmt signaling, and targeted therapy in metastasis tumor

Mitochondrial dysfunction, UPRmt signaling, and targeted therapy in metastasis tumor

A influência dos polimorfismos CYP1A1 A4889G, CYP1A1 T6235C, NQO1 C609T e GSTP1 Ile105Val e da deleção homozigótica de GSTM1 e GSTT1 no risco e prognóstico dos pacientes com linfoma não-Hodgkin difuso de grandes células B

Roles of dioxins and heavy metals in cancer and neurological diseases using ROS-mediated mechanisms

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