<i>Rb</i> is critical in a mammalian tissue stem cell population

Wenzel, Pamela L.; Wu, Lizhao; Bruin, Alain de; Chong, Jean Leon; Chen, Wen Yi; Dureska, Geoffrey; Sites, Emily; Pan, Tony; Sharma, Ashish; Huang, Kun; Ridgway, Randall; Mosaliganti, Kishore; Sharp, Richard; Machiraju, Raghu; Saltz, Joel; Yamamoto, Hideyuki; Cross, James C.; Robinson, Michael L.; Leone, Gustavo

doi:10.1101/gad.1485307

Cited by 80 publications

(100 citation statements)

References 49 publications

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“…14 However, this concept was difficult to reconcile with the amelioration of Rb-null erythroid defects in mice provided with a wild-type placenta but harboring Rb-null macrophages. 9 Our current work provides an explanation for these seemingly contradictory results by showing that Rb-null macrophages harvested from healthy fetal liver or bone marrow are not defective for erythroblast island formation in the absence of exogenous stress, that hypoxia can disrupt erythroblast islands in vitro, that macrophage coculture does not affect the level of red cell enucleation, and that the Rb-null fetal liver is hypoxic at times when erythroid islands are increasing in size and number in wild-type fetal liver. 4 Thus, erythroblastic island defects in Rb-null mice and in ex vivo islands derived from these mice likely stem from the deleterious effects on macrophage-erythroblast interactions by hypoxia and the rapidly deteriorating microenvironment.…”

Section: Discussionmentioning

confidence: 99%

“…The induction of known HIF target genes in the E12.5 Rb-null fetal liver is consistent with ischemia (due to placental defects and anemia) being the cause, as opposed to the consequence, of the cell death that is first detected in E13.5 Rb-null fetal liver. 8,9,12 We also used the microarray data and quantitative real-time PCR to examine how loss of Rb affected expression of macrophagespecific genes that had been previously implicated in the erythroblast island defect in Rb-null fetal liver, 14 including c-Fms, myeloperoxidase (MPO), cathepsin S, complement components, We noted that Rb-null erythroblasts (D) failed to enucleate irrespective of macrophage contacts (arrow) and demonstrated increased size and abnormal chromatin structure as reported previously. 11,12 (E,F) Native erythroblast islands cultured in vitro from mice with the indicated Rb genotypes and at early or later stages of embryonic development were enumerated (F).…”

Section: Hypoxia Disrupts Erythroblast Island Formation Independent Omentioning

confidence: 99%

“…7 Mice carrying a targeted deletion of the Rb tumor suppressor gene in their germ line die at E13.5 to E14.5 of gestation, exhibiting extensive cell death in multiple tissues, including the fetal liver, and this has been attributed to systemic ischemia due to defective placental function and anemia. 8,9 The production of enucleated mature red blood cells appeared normal in mice derived from germ-line Rb-null chimeras 10 and in conditionally targeted E15.5 embryos in which Rb was not deleted in the placenta. 8 However, analysis of erythroblast maturation in vitro 11,12 or in Rb-null chimeric mice that had been challenged in vivo with phenylhydrazine to induce stress erythropoiesis recapitulated the erythroid maturation defects seen previously in the developing Rb-null fetal liver, including the failure to enucleate and up-regulate TER119.…”

Section: Introductionmentioning

confidence: 99%

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Hypoxic stress underlies defects in erythroblast islands in the Rb-null mouse

Dibling¹,

Macleod

2007

Blood

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Definitive erythropoiesis occurs in islands composed of a central macrophage in contact with differentiating erythroblasts. Erythroid maturation including enucleation can also occur in the absence of macrophages both in vivo and in vitro. We reported previously that loss of Rb induces cell-autonomous defects in red cell maturation under stress conditions, while other reports have suggested that the failure of Rb-null erythroblasts to enucleate is due to defects in associated macrophages. Here we show that erythropoietic islands are disrupted by hypoxic stress, such as occurs in the Rb-null fetal liver, that Rb ؊/؊ macrophages are competent for erythropoietic island formation in the absence of exogenous stress and that enucleation defects persist in Rb-null erythroblasts irrespective of macrophage function.

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Section: Discussionmentioning

confidence: 99%

Section: Hypoxia Disrupts Erythroblast Island Formation Independent Omentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Hypoxic stress underlies defects in erythroblast islands in the Rb-null mouse

Dibling¹,

Macleod

2007

Blood

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“…Thus, the RB pathway controls cellular processes that are critically linked to stem cell properties. Accordingly, RB and its two family members p107 and p130 are important regulators of adult stem cell and progenitor populations [10][11][12][13][14][15] .…”

mentioning

confidence: 99%

The RB family is required for the self-renewal and survival of human embryonic stem cells

2012

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The mechanisms ensuring the long-term self-renewal of human embryonic stem cells are still only partly understood, limiting their use in cellular therapies. Here we found that increased activity of the RB cell cycle inhibitor in human embryonic stem cells induces cell cycle arrest, differentiation and cell death. Conversely, inactivation of the entire RB family (RB, p107 and p130) in human embryonic stem cells triggers G2/M arrest and cell death through functional activation of the p53 pathway and the cell cycle inhibitor p21. Differences in E2F target gene activation upon loss of RB family function between human embryonic stem cells, mouse embryonic stem cells and human fibroblasts underscore key differences in the cell cycle regulatory networks of human embryonic stem cells. Finally, loss of RB family function promotes genomic instability in both human and mouse embryonic stem cells, uncoupling cell cycle defects from chromosomal instability. These experiments indicate that a homeostatic level of RB activity is essential for the self-renewal and the survival of human embryonic stem cells.

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“…In order to evaluate our optimization techniques and implementation methods, we applied our registration algorithm to a series of microscopic images of consecutive sections of (1) mouse placenta for a morphometric study on the role of the retinoblastoma gene and (2) mammary gland for studying the breast cancer tumor microenvironment [16]. For details about these sets of images, see Table 5.…”

Section: Input Data Setmentioning

confidence: 99%

Non-rigid Registration for Large Sets of Microscopic Images on Graphics Processors

Ruiz

Ujaldón

Cooper

et al. 2008

J Sign Process Syst Sign Image Video Technol

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Microscopic imaging is an important tool for characterizing tissue morphology and pathology. 3D reconstruction and visualization of large sample tissue structure requires registration of large sets of high-resolution images. However, the scale of this problem presents a challenge for automatic registration methods. In this paper we present a novel method for efficient automatic registration using graphics processing units (GPUs) and parallel programming. Comparing a C++ CPU implementation with Compute Unified Device Architecture (CUDA) libraries and pthreads running on GPU we achieve a speed-up factor of up to 4.11× with a single GPU and 6.68× with a GPU pair. We present execution times for a benchmark composed of two sets of large-scale images: mouse placenta (16K × 16K pixels) and breast cancer tumors (23K × 62K pixels). It takes more than 12 hours for the genetic case in C++ to register a typical sample composed of 500 consecutive slides, which was reduced to less than 2 hours using two GPUs, in addition to a very promising scalability for extending those gains easily on a large number of GPUs in a distributed system.

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Rb is critical in a mammalian tissue stem cell population

Cited by 80 publications

References 49 publications

Hypoxic stress underlies defects in erythroblast islands in the Rb-null mouse

Hypoxic stress underlies defects in erythroblast islands in the Rb-null mouse

The RB family is required for the self-renewal and survival of human embryonic stem cells

Non-rigid Registration for Large Sets of Microscopic Images on Graphics Processors

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