Fang-Pei Chang scite author profile

Although JC virus (JCV), a human polyomavirus, has been detected in colon cancers, the association between JCV and colon cancer remains controversial. In Taiwan, the prevalence of JCV infection in colon cancer patients has not been reported. Thus, the purpose of this study was to investigate JCV infection in colon cancers in Taiwan. Formalin-fixed, paraffin-embedded tissues from 22 colon cancer patients were examined in this study. Nested PCR was performed to detect viral genomic DNA. The product of the nested PCR flanking the JCV regulatory region was sequenced further. Viral large tumor protein, LT, and late capsid protein, VP1, were examined by immunohistochemistry (IHC). Nested PCR revealed JCV genomic DNA in 86.4% (19/22) of the colon cancer tissue samples. Both rearranged and archetypal genotypes of JCV were identified. Expression of JCV LT was positive in 63.6% (14/22) of the examined colon cancer tissue samples but not in any adjacent normal region. Expression of viral capsid protein VP1 was not detected in any of the tissues examined. The current study demonstrates that JCV genomic DNA was present in the examined colon cancer tissues. The genotypes of JCV in colon cancer tissues were also identified. Expression of viral early protein but not structural capsid protein was detected in the examined colon cancer tissues. Furthermore, a high prevalence of JCV infection in colon cancer tissues in Taiwan was also demonstrated.

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Cyclin D1 acts as a barrier to pluripotent reprogramming by promoting neural progenitor fate commitment

Chen

Wang

Yan

et al. 2014

FEBS Letters

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Edited by Ned Mantei Keywords:Induced pluripotent stem cell Induced neural stem/progenitor cell Cyclin D Cell cycle a b s t r a c t A short G1 phase is a characteristic feature of the cell cycle structure of pluripotent cells, and is reestablished during Yamanaka factor-mediated pluripotent reprogramming. How cell cycle control is adjusted to meet the requirements of pluripotent cell fate commitment during reprogramming is less well understood. Elevated levels of cyclin D1 were initially found to impair pluripotency maintenance. The current work further identified Cyclin D1 to be capable of transcriptionally upregulating Pax6, which promoted reprogramming cells to commit to a neural progenitor fate rather than a pluripotent cell fate. These findings explain the importance of reestablishment of G1-phase restriction in pluripotent reprogramming.

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Protoporphyrin IX accumulation disrupts mitochondrial dynamics and function in ABCG2‐deficient hepatocytes

Lin

Chang

et al. 2013

FEBS Letters

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a b s t r a c tTargeted inhibition of multidrug ABCG2 transporter is believed to improve cancer therapeutics. However, the consequences of ABCG2 inhibition have not been systematically evaluated since ABCG2 is expressed in several organs including the liver. Here, we demonstrate that ABCG2-deficient hepatocytes have increased amounts of fragmental mitochondria accompanied by disruption of mitochondrial dynamics and functions. This disruption was due to ABCG2 knockout elevating intracellular protoporphyrin IX, which led to upregulation of DRP-1-mediated mitochondrial fission. The finding that ABCG2 deficiency can generate dysfunctional mitochondria in hepatocytes raises concerns regarding the systematic use of ABCG2 inhibitor in cancer patients.

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CHAC2 is essential for self-renewal and glutathione maintenance in human embryonic stem cells

Wang

Yang

Hsu

et al. 2017

Free Radical Biology and Medicine

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Fang-Pei Chang

Prevalence and genotype identification of human JC virus in colon cancer in Taiwan

Cyclin D1 acts as a barrier to pluripotent reprogramming by promoting neural progenitor fate commitment

Protoporphyrin IX accumulation disrupts mitochondrial dynamics and function in ABCG2‐deficient hepatocytes

CHAC2 is essential for self-renewal and glutathione maintenance in human embryonic stem cells

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