A MicroRNA Signature of Hypoxia

Kulshreshtha, Ritu; Ferracin, Manuela; Wojcik, Sylwia E.; Garzon, Ramiro; Alder, Hansjüerg; Agosto-Perez, Francisco; Davuluri, Ramana V.; Liu, Chang Gong; Croce, Carlo M.; Negrini, Massimo; Calin, George A.; Ivan, Mircea

doi:10.1128/mcb.01395-06

Cited by 965 publications

(950 citation statements)

References 31 publications

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“…The HRM group includes: miR-21, 23a, 23b, 24, 26a, 26b, 27a, 30b, 93, 103, 103, 106a, 107, 125b, 181a, 181b, 181c, 192, 195, 210 and 213, which were consistently induced in response to hypoxia in the breast and colon cancer cells tested. 21 Our study selected only microRNAs exhibiting consistent upregulation in at least two cell lines and at several time points in hypoxia, potentially increasing the stringency of the screen. Three additional articles reported microRNAs that respond to low oxygen with some notable similarities, including miR-210, miR-30b, 93 and 181b.…”

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

“…[22][23][24] It is also true, however, that a significant number of microRNAs differed between the studies, which is not necessarily surprising, given the differences in the cellular backgrounds and technology employed, both being a recognized source of variability. An additional difference was in the experimental conditions employed by the different groups: hypoxia mimetics, 22 versus 1% oxygen for 1 h, 23 versus 5% oxygen for 8 h, 23 versus 0.2% for various periods of time from 8-48 h. 21 In addition to the microRNAs that respond to hypoxia by upregulation, a set of microRNAs were identified as downregulated in hypoxic cells, including miR-15b, 16, 19a, 20a, 20b, 29b, 30b, 30e-5p, 101, 141, 122a, 186, 320 and 197. [22][23][24] In our study, we have also detected microRNAs that exhibited downregulation at the level of microarrays (miR-126, 128, 138, 323, 326); however, the changes seemed restricted to one cell line and were not pursued at this stage (R Kulshreshtha et al, unpublished).…”

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

“…The strategy employed a combination of HIF transduction, chromatin immunoprecipitation and luciferase-based reporters driven by fragments of select HRM promoters. 21 Delineating the promoter regions of microRNAs, where relevant transcription factors such as HIF bind, is a necessary step for an expanded understanding of microRNA expression control. The main challenge comes from the fact that only few microRNA promoters have been identified experimentally.…”

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

“…[25][26][27] In a preliminary analysis of the promoters of all known and predicted microRNAs, we predicted HIF-binding sites by position weight matrix approach. 21 While our methodology analyzed the 5 kb promoter region of all the microRNAs, the promoter regions can span much longer regions. The analysis, performed separately for individual types of HIFbinding consensuses (V$HIF_Q3 and V$HIF_Q5) revealed that the HRMs (as a group) contains significantly more microRNAs with at least one HIF site than the average random 23 microRNAs.…”

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

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A microRNA component of the hypoxic response

et al. 2008

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microRNAs participate in a wide variety of physiological and pathological cellular processes. Recent studies have established a link between a specific group of microRNAs and hypoxia, a key feature of the neoplastic microenvironment. A significant proportion of the hypoxia-regulated microRNAs (HRMs) are also overexpressed in human cancers, suggesting a role in tumorigenesis. Preliminary evidence suggests that they could affect important processes such as apoptosis, proliferation and angiogenesis. Several HRMs exhibit induction in response to HIF activation, thus extending its repertoire of targets beyond translated genes. In the present review, we discuss the emerging roles of HRMs in oxygen deprivation in cancer context.

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Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

Section: Small Size Regulators With Far-reaching Impactmentioning

confidence: 99%

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A microRNA component of the hypoxic response

et al. 2008

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“…Recent evidence indicates that hypoxia induces the synthesis of microRNAs (MIRs), which add additional levels of complexity in the regulation of gene expression under hypoxia [3,4]. MIRs, a group of small RNAs with approximately 22 nucleotides in length, have important roles in the regulation of gene expression.…”

Section: Hypoxia Signaling In the Lungmentioning

confidence: 99%

Hypoxia and chronic lung disease

et al. 2007

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The lung is both the conduit for oxygen uptake and is also affected by hypoxia and hypoxia signaling. Decreased ventilatory drive, airway obstructive processes, intra-alveolar exudates, septal thickening by edema, inflammation, fibrosis, or damage to alveolar capillaries will all interpose a significant and potentially life-threatening barrier to proper oxygenation, therefore enhancing the alveolar/arterial pO 2 gradient. These processes result in decreased blood and tissue oxygenation. This review addresses the relationship of hypoxia with lung development and with lung diseases. We particularly focus on molecular mechanisms underlying hypoxia-driven physiological and pathophysiological lung processes, specifically in the infant lung, pulmonary hypertension, and chronic obstructive pulmonary disease.Keywords Hypoxia . Lung . Pathology . HIF Air, containing oxygen at approximately 21% partial pressure at sea level (140-150 mmHg), travels through up to 20 generations of airways by mass flow and then diffuses into the gas exchange units (alveoli) in the lung with a partial pressure of approximately 105-110 mmHg. The human lung contains approximately 480 million alveoli, which represent 64% of total lung structure. These alveoli are elegantly packed in only 1.3-2.6 L of total lung volume, providing a surface area of 120-150 m 2 , equivalent to the dimensions of a "tennis court" dedicated for gas exchange. Although the molecular determinants of lung size are not known, oxygen diffusion constant and gas exchange surface area are roughly proportional to body weight and oxygen consumption in different species [1]. Physical hyperactivity and exposure to a cold environment or high altitude lead to increased oxygen diffusion capacity, in proportion to enhanced oxygen consumption [1].Decreased ventilatory drive, airway obstructive processes, intraalveolar exudates, septal thickening by edema, inflammation, fibrosis, or damage to alveolar capillaries will all interpose a significant and potentially life-threatening barrier to proper oxygenation, therefore enhancing the alveolar/ arterial pO 2 gradient. This review addresses the contribution of hypoxia to lung diseases and the potential molecular mechanisms involved in hypoxia-driven physiological and pathophysiological lung processes (Fig. 1), particularly in the infant lung, pulmonary hypertension, and chronic obstructive pulmonary disease. The fundamental concepts underlying hypoxia-induced gene expression and the molecular regulation of HIF(s) also apply to the lung, and they will be cited in relation to their demonstrated role in lung physiology or pathophysiology.

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Vascular‐Targeted Molecular Therapy

Dougherty

2010

Tumor Microenvironment

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A MicroRNA Signature of Hypoxia

Cited by 965 publications

References 31 publications

A microRNA component of the hypoxic response

A microRNA component of the hypoxic response

Hypoxia and chronic lung disease

Vascular‐Targeted Molecular Therapy

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