Circulating tumor DNA in blood: Future genomic biomarkers for cancer detection

Sumbal, Sumbal; Javed, Aneeqa; Afroze, Bakht; Zulfiqar, Hafiza Fizzah; Javed, Faqeeha; Noreen, Sobia; Ijaz, Bushra

doi:10.1016/j.exphem.2018.06.003

Cited by 35 publications

(27 citation statements)

References 55 publications

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“…They consisted of 160–180 bp, indicating the degradation of DNA to nucleosomal units that is considered as properties of the apoptotic process [ 160 , 161 ]. It has been revealed that CTCs has less sensitivity for detection of tumor related genetic rearrangements in comparison with ctDNA, due to low detectable number of CTCs in blood circulation [ 157 ]. Determining tumor proliferation and metastases in CTCs are performed using DNA methylation [ 162 ].…”

Section: Identifying Os Stem Cell Populations As Therapeutic Targetsmentioning

confidence: 99%

“…The ctDNA analysis as liquid biopsy provides an opportunity to accurately assess the status of cancer patients with a much cheaper, faster, and reliable method, because ctDNA serve as promising diagnostic, prognostic, and predictive marker. In addition to commonly used DNA recognition methods, including PCR, real-time PCR, Digital PCR based techniques (e.g., droplet digital PCR), PARE and BEAMing, [ 157 , 164 , 165 ]. Recent developments in Next Generation Sequencing (NGS) provide a new method for ctDNA investigation.…”

Section: Identifying Os Stem Cell Populations As Therapeutic Targetsmentioning

confidence: 99%

“…CtDNA can also be used as a medical tool available to physicians for changing current approach in personalized cancer management, since it is capable of providing accurate data about each patient. However, this technique still needs further optimization [ 157 , 164 ].…”

Section: Identifying Os Stem Cell Populations As Therapeutic Targetsmentioning

confidence: 99%

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Novel molecular insights and new therapeutic strategies in osteosarcoma

et al. 2018

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Osteosarcoma (OS) is one of the most prevalent malignant cancers with lower survival and poor overall prognosis mainly in children and adolescents. Identifying the molecular mechanisms and OS stem cells (OSCs) as new concepts involved in disease pathogenesis and progression may potentially lead to new therapeutic targets. Therefore, therapeutic targeting of OSCs can be one of the most important and effective strategies for the treatment of OS. This review describes the new molecular targets of OS as well as novel therapeutic approaches in the design of future investigations and treatment.

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Section: Identifying Os Stem Cell Populations As Therapeutic Targetsmentioning

confidence: 99%

Section: Identifying Os Stem Cell Populations As Therapeutic Targetsmentioning

confidence: 99%

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Novel molecular insights and new therapeutic strategies in osteosarcoma

et al. 2018

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“…Ответные реакции организма на опухоль, как и ее развитие, это многообразный, многоуровневый процесс, который отражает изменения, происходящие при злокачественной трансформации как на клеточном, так и субклеточном уровнях, а также в органах и системах, вовлеченных в канцерогенез. В частности, нарушение гомеостаза на генном уровне влечет за собой изменение функционирования различных каскадов сигнальных путей и молекул, что приводит к нарушениям иммунных процессов, метаболическим, энергетическим сдвигам и находит свое отражение в виде изменений в соматических немалигнизированных клетках, появлении опухоль-ассоциированных сывороточных маркеров, таких как С-реактивный белок, лактатдегидрогеназа, лактат, и циркулирующих в крови генетических (ДНК) и эпигенетических (микроРНК) маркеров, чему посвящены многочисленные публикации [2][3][4][5][6][7].…”

Section: Introductionunclassified

Современное Развитие Направления — Цитологическая Реактивность Больного Онкологического Профиля

2020

clinicaloncology

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“…Circulating tumour DNA (ctDNA) is an emerging biomarker for cancer which has the potential for early detection and monitoring of treatment response [1]. Rapid and accurate detection of important mutations, for example, tumour protein 53 (TP53), from the ctDNA fraction in a point-of-care (PoC) manner represents a significant analytical challenge.…”

Section: Introductionmentioning

confidence: 99%

Establishing a Field-Effect Transistor Sensor for the Detection of Mutations in the Tumour Protein 53 Gene (TP53)—An Electrochemical Optimisation Approach

et al. 2019

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We present a low-cost, sensitive and specific DNA field-effect transistor sensor for the rapid detection of a common mutation to the tumour protein 53 gene (TP53). The sensor consists of a commercially available, low-cost, field-effect transistor attached in series to a gold electrode sensing pad for DNA hybridisation. The sensor has been predominantly optimised electrochemically, particularly with respect to open-circuit potentiometry as a route towards understanding potential (voltage) changes upon DNA hybridisation using a transistor. The developed sensor responds sensitively to TP53 mutant DNA as low as 100 nM concentration. The sensor responds linearly as a function of DNA target concentration and is able to differentiate between complementary and noncomplementary DNA target sequences.

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Circulating tumor DNA in blood: Future genomic biomarkers for cancer detection

Cited by 35 publications

References 55 publications

Novel molecular insights and new therapeutic strategies in osteosarcoma

Novel molecular insights and new therapeutic strategies in osteosarcoma

Современное Развитие Направления — Цитологическая Реактивность Больного Онкологического Профиля

Establishing a Field-Effect Transistor Sensor for the Detection of Mutations in the Tumour Protein 53 Gene (TP53)—An Electrochemical Optimisation Approach

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