Tissue Microarray Cytometry Reveals Positive Impact of Homeodomain Interacting Protein Kinase 2 in Colon Cancer Survival Irrespective of p53 Function

Soubeyran, Isabelle; Mahouche, Isabelle; Grigoletto, Aude; Lesté-Lasserre, Thierry; Drutel, Guillaume; Rey, Christophe; Pédeboscq, S.; Brouste, Véronique; Sabourin, Jean‐Christophe; Bécouarn, Y.; Ichas, François; Giorgi, Francesca De

doi:10.1016/j.ajpath.2011.01.021

Cited by 14 publications

(10 citation statements)

References 28 publications

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“…It was recently shown that changes in the expression levels of HIPK2 between the normal and tumor tissue of each colorectal carcinoma patient have a positive effect on survival, irrespective of p53 function, raising the possibility of a p53‐independent apoptotic modulation 33. However, this study found no significant difference in the range of expression level in the tumors compared with the normal mucosa or in a subgroup of tumors 33…”

Section: Discussioncontrasting

confidence: 70%

Zinc supplementation augments in vivo antitumor effect of chemotherapy by restoring p53 function

Margalit

Simon

Yakubov

et al. 2011

Intl Journal of Cancer

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Activated p53 is necessary for tumor suppression. Homeodomain-interacting protein kinase-2 (HIPK2) is a positive regulator of functional p53. HIPK2 modulates wild-type p53 activity toward proapoptotic transcription and tumor suppression by the phosphorylation of serine 46. Knock-down of HIPK2 interferes with tumor suppression and sensitivity to chemotherapy. Combined administration of adriamycin and zinc restores activity of misfolded p53 and enables the induction of its proapoptotic and tumor suppressor functions in vitro and in vivo. We therefore looked for a cancer model where HIPK2 expression is low. MMTV-neu transgenic mice overexpressing HER2/neu, develop mammary tumors at puberty with a long latency, showing very low expression of HIPK2. Here we show that whereas these tumors are resistant to adriamycin treatment, a combination of adriamycin and zinc suppresses tumor growth in vivo in these mice, an effect evidenced by the histological features of the mammary tumors. The combined treatment of adriamycin and zinc also restores wild-type p53 conformation and induces proapoptotic transcription activity. These findings may open up new possibilities for the treatment of human cancers via the combination of zinc with chemotherapeutic agents, for a selected group of patients expressing low levels of HIPK2, with an intact p53. In addition, HIPK2 may serve as a new biomarker for tumor aggressiveness.

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Section: Discussioncontrasting

confidence: 70%

Zinc supplementation augments in vivo antitumor effect of chemotherapy by restoring p53 function

Margalit

Simon

Yakubov

et al. 2011

Intl Journal of Cancer

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“…We found that HIPK2 expression markedly decreased in invasive carcinomas, whereas it was highly expressed in preinvasive lesions. In addition, Soubeyran et al 19 has shown that the increased expression of the HIPK2 protein in colorectal tumor cells compared with paired normal tissue cells has a strong impact on better survival in patients with colorectal cancer. DOrazi et al 18 also reported that HIPK2 knockdown strongly correlates with increased tumor growth in colorectal cancer in vitro.…”

Section: Discussionmentioning

confidence: 99%

“…DOrazi et al 18 also reported that HIPK2 knockdown strongly correlates with increased tumor growth in colorectal cancer in vitro. In addition, Soubeyran et al 19 has shown that the increased expression of the HIPK2 protein in colorectal tumor cells compared with paired normal tissue cells has a strong impact on better survival in patients with colorectal cancer. The authors concluded that HIPK2 depletion is associated with tumor development and progression.…”

Section: Discussionmentioning

confidence: 99%

HIPK2 expression in progression of cutaneous epithelial neoplasm

et al. 2015

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“…Genomic DNAs were used to determine p53 mutational status by sequencing, while RNA extracts were used to quantify p21 transcript levels by qRT-PCR. 14 The TMA was done to contain one core of normal mucosa (punched far away JNK/p38 kinases (as proposed above) were supposedly induced. It is still puzzling to understand why and how HIPK1 specifically targets serine 15.…”

Section: Methodsmentioning

confidence: 99%

“…Various studies implicate HIPK1 in carcinogenesis, but it is still difficult to assign a pro-or anti-tumoral role to it, and even more to find convincing in vivo data. To fill this gap, we used a TMA (previously generated in our laboratory), 14 composed of both normal and tumoral tissue from 80 colorectal cancer (CRC) patients, and compared HIPK1 expression levels in each type of sample after immunohistochemical staining (Fig. 1A-C).…”

Section: Hipk1mentioning

confidence: 99%