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2009年07月14日

【期刊论文】Age-dependent and iron-independent expression of two mRNA isoforms of divalent metal transporter 1 in rat brain

段相林, Ya Ke a, b, c, Yan Zhong Chang a, Xiang Lin Duan a, Jin Rong Du a, Li Zhu a, Kui Wang b, Xiao Da Yang b, Kwok Ping Ho a, Zhong-ming Qian a, d, ∗

Neurobiology of Aging 26(2005)739-748,-0001,():

-1年11月30日

摘要

The DMT1(Nramp2/DCT1) is a newly discovered proton-coupled metal-ion transport protein. The cellular localization and functional characterization of DMT1 suggest that it might play a role in physiological iron transport in the brain. In the study, we evaluated effects of dietary iron and age on iron content and DMT1 expression in four brain regions: cortex, hippocampus, striatum, substantia nigra. Total iron content in all regions was significantly lower in the low-iron diet rats and higher in the high-iron diet rats than that in the control animals, showing that dietary iron treatment for 6-weeks can alter brain iron levels. Contrary to our expectation, there was no significant alternation in DMT1(+IRE) and (−IRE) mRNA expression and protein content in all brain regions examined in spite of the existence of the altered iron levels in these regions after 6-weeks’ diet treatment although TfR mRNA expression and protein level were affected significantly, as was expected. The data demonstrates that expression of DMT1(+IRE) and (−IRE) was not regulated by iron in these regions of adult rats. The lack of response of DMT1 to iron status in the brain suggests that the IRE of brain DMT1 mRNA might be not really iron-responsive and that DMT1-mediated iron transport might be not the rate-limiting step in brain iron uptake in adult rats. Our findings also showed that development can significantly affect brain iron and DMT1(+IRE) and (−IRE) expression but the effect varies in different brain regions, indicating a regionally specific regulation in the brain.

Brain iron metabolism, DMT1(, Nramp2/, DCT1), expression, Age and iron status, Brain regions

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2009年07月14日

【期刊论文】Post-Transcriptional Expression of DMT1 in the Heart of Rat

段相林, YA KE, YIN YIN CHEN, YAN ZHONG CHANG, , XIANG LIN DUAN, KWOK PING HO, DE HE JIANG, KUI WANG, AND ZHONG MING QIAN, *

JOURNAL OF CELLULAR PHYSIOLOGY 196(2003)124-130,-0001,():

-1年11月30日

摘要

Non-transferrin-bound iron (NTBI) overtaken by heart cells might be a key cause leading to iron-mediated injury in heart disorders. NTBI uptake by heart cells might be mediated by divalent metal transporter 1 (DMT1). The understanding of the role ofDMT1in heart iron metabolism is fundamental for elucidating the cause resulting in excessive iron in the heart. The study was to evaluate effects of age and dietary iron on DMT1 mRNA expression and protein synthesis in rat heart. DMT1 mRNA expression was determined by RT-PCR and sequence analysis, and DMT1 protein by Western blot analysis. DMT1 mRNAs with or without iron-responsive element (IRE) both were found in rat heart. Expression of two forms ofDMT1mRNAs was the lowest at the age of post-natal day (PND) 7, and then increased with the age, reaching the highest at PND196 (non-IRE form) and PND63 (IRE form), respectively. During different ages, the levels ofDMT1(IRE)mRNAwere higher than those ofDMT1(non-IRE)mRNAand were significantly correlated with the non-heme iron contents in the heart. After fed a high iron for 6 weeks, the rats had a sixfold elevation in heart iron and 22% (non-IRE from) and 40% (IRE from) reduction in DMT1protein compared to the controls. Alow iron diet for 6-weeks caused cardiac hypertrophy and heart iron deficiency and also an increase in levels of two forms of DMT1 proteins. However, iron status had no significant effect on DMT1 (IRE) and DMT1 (non-IRE) mRNAs expression in the heart, although it can significantly influence heart transferrin receptor (TfR) mRNA expression. The results demonstrated that DMT1 mRNAs expression in the heart is age-dependent and that two forms of DMT1 mRNAs both are regulated by iron on the post-transcriptional level only.

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    河北师范大学,河北

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