Prognostic significance of NPM1 mutation-modulated microRNA-mRNA regulation in acute myeloid leukemia.

Distinct microRNA (miRNA) and mRNA signatures were reported in nucleophosmin (NPM1)-mutated acute myeloid leukemia (AML). However, it remains unknown whether the mutation participates in the dynamic interaction between miRNA and mRNA. In this study, we aimed to investigate the role of NPM1 mutation in modulating miRNA-mRNA regulation (MMR). From the sample-paired miRNA/mRNA microarrays of 181 de novo AML patients, we found that MMR was dynamic and could be affected by NPM1 mutation. By a systematic framework, we identified 493 NPM1 mutation-modulated MMR pairs, where the strength of MMR was significantly attenuated in patients carrying NPM1 mutations, compared to those with wild-type NPM1. These miRNAs/mRNAs were associated with pathways implicated in cancer and known functions of NPM1 mutation. Such modulation of MMR was validated in two independent cohorts as well as in cells with different NPM1 mutant burdens. Furthermore, we showed that the regulatory strength of nine MMR pairs could predict patients' outcomes. Combining these pairs, a scoring system was proposed and shown to predict survival in discovery and validation data sets, independent of other known prognostic factors. Our study provides novel biological insights into the role of NPM1 mutation as a modulator of MMR, based on which a novel prognostic marker is proposed in AML.

Prenatal smoke exposure, DNA methylation, and childhood atopic dermatitis.

BACKGROUND: The biological mechanisms of how prenatal smoke exposure leading to atopic disorders remain to be addressed. Whether prenatal smoke exposure affects DNA methylation leading to atopic disorders is not clear. OBJECTIVE: As most children suffering from atopic dermatitis (AD) continue to develop asthma later in life, we explored whether prenatal smoke exposure induces cord blood DNA methylation. METHODS: Methylation differences associated with smoke exposure were screened by Illumina Infinium 27K methylation arrays for 14 children from the Taiwan birth panel study cohort initially. Information about development of atopic dermatitis (AD) and risk factors was collected. Cord blood cotinine levels were measured to represent prenatal smoke exposure. CpG loci that demonstrated a statistically significant difference in methylation were validated by methylation-dependent fragment separation (MDFS). Differential methylation in three genes (TSLP, GSTT1, and CYB5R3) was identified through the screen. RESULTS: Among these, only thymic stromal lymphopoietin (TSLP) gene displayed significant difference in promoter methylation percentage after being validated by MDFS (p = 0.018). TSLP gene was further investigated in a larger sample of 150 children from the cohort who completed the follow-up study. Methylation status of the TSLP 5'-CpG island (CGI) was found to be significantly associated with prenatal smoke exposure (OR = 3.17, 95% CI = 1.63-6.19) and with AD (OR = 2.32, 95% CI = 1.06-5.11). The degree of TSLP 5'CGI methylation inversely correlated with TSLP protein expression levels (r = -0.45, P = 0.001). CONCLUSIONS & CLINICAL RELEVANCE: The effect of prenatal tobacco smoke exposure on the risk for AD may be mediated through DNA methylation.

[Calcium ion-selective miroelectrodes for measurement of free calcium in saliva]

In this paper, the free calcium concentration in saliva was measured and evaluated by the neutral carries ion-selective microelectrodes.The statistical results showed that there was no significant difference (the groups of all,P>0.05) between children and adult,between male children and female one,between caries-free and caries-active,and between interval of two weeks.The results suggested that caries might be no direct relation to the calcium concentration in children physiological saliva. Calcium ion-selective microelectrodes seems to be a good method for measuring free calcium in oral micro-sample fluid.

[Study and application of atropine field-effect transistor].

Atropine-H2SO4 is widely used in clinic. The atropine sensitive electrode has been prepared, but Atropine field-effect transistor (Atropine-FET) has not been reported. In this communication, electro-active material is atropine tetraphenylboron. The sensor was fabricated by coating solution composed of electro-active material, dibutyl phthalate (DBP) and 5% PVC in tetrahydrofuran (THF) on Pt wire of gate electrode of MOSFET. The sensor showed linear response to atropine within concentration range 2.0 x 10(-2)-6.3 x 10(-5) mol/L. The slope of the sensor was 55 mV/decade and the limit of detection was 1.6 x 10(-5) mol/L. The sensor response was not affected by pH in the range 3.2-8.2, and the sensor can be used for the determination of atropine sulphate in drug-substances by direct potentiometry. The results of determination were in agreement with the data obtained by the official method in Chinese Pharmacopoeia. The method appears to be a rapid, simple and precise one.