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In Development this week (Vol. 138, Issue 5)

Posted by , on 8 February 2011

Here are the highlights from the current issue of Development:

From pluripotent to pancreatic fates

A reliable method for generating insulin-producing β-cells from human pluripotent stem cells (hPSCs) would provide new therapeutic options for people with diabetes. So far, no-one has developed such a method but, on p. 861, Gordon Keller and colleagues provide new insights into the complex signalling networks that underlie β-cell differentiation. The generation of β-cells from hPSCs requires efficient endoderm induction followed by patterning and specification to a pancreatic fate. The researchers show that the duration of nodal/activin A signalling plays a pivotal role in endoderm induction and that WNT signalling enhances the subsequent development of pancreatic lineage cells. Inhibition of BMP signalling at specific stages is also essential for the generation of insulin-expressing cells. Importantly, report the researchers, optimal stage-specific manipulation of TGFβ and WNT signalling yields cell populations that produce insulin at levels similar to those made by the pancreas. However, because these cells also make other hormones, further studies are needed to discover how to convert these polyhormonal cells into functional β-cells.

Full Fat signalling in mammals: Dchs1 and Fat4 pair up

In Drosophila, Dachsous and Fat act as ligand and receptor, respectively, for a signalling pathway that regulates planar cell polarity (PCP) and transcription via the Hippo pathway. Mammals encode multiple Fat and Dachsous proteins but do they have an equivalent Fat signalling pathway? On p. 947, Yaopan Mao and colleagues report that murine Dchs1 and Fat4 function as a ligand-receptor pair during development. The researchers show that Dchs1 and Fat4 single mutants and Dchs1 Fat4 double mutants exhibit similar phenotypes. These phenotypes include the formation of kidney cysts and cochlear defects, suggesting that Dchs1-Fat4 signalling influences PCP in mice. However, the researchers also identify non-PCP-related requirements for Dchs1-Fat4 signalling in the development of other organs. In particular, they show that Dchs1 and Fat4 are needed for growth, branching and cell survival during early kidney development. Together, these results identify Dchs1 and Fat4 as a ligand-receptor pair for mammalian Fat signalling and identify new requirements for Fat signalling in multiple organs.

Capicua mediates response to RTK signalling

Receptor tyrosine kinase (RTK) signalling pathways regulate many developmental decisions, but how RTK signalling controls the expression of its target genes in different contexts is poorly understood. Here, Gerardo Jiménez and co-workers reveal that octameric DNA-binding sites for the transcriptional repressor Capicua (Cic) are critically involved in RTK signalling in Drosophila (see p. 915). They show that the regulation of terminal gap gene expression by the Drosophila RTK Torso in early embryos depends on octameric Cic-binding sites in the enhancer region of the gap gene huckebein. Moreover, these Cic-binding motifs are essential for recruitment of the Groucho co-repressor to the huckebein enhancer in vivo. Cic-binding sites also respond to EGFR RTK pathway activation in the embryonic neuroectoderm and in the developing wing. Finally, using synthetic enhancer constructs, the researchers show that Cic-binding motifs provide the regulatory information necessary to translate RTK signalling inputs into precise transcriptional responses in different tissues. Thus, they conclude, octameric Cic-binding motifs are general response elements for RTK signalling in Drosophila.

A new spin(dle) on stem cell division

Stem cells divide asymmetrically to balance self-renewal and differentiation, thereby maintaining tissue homeostasis. But what coordinates the divisions of multiple stem cell populations in complex tissues? To address this question, Yukiko Yamashita, Alan Hunt and colleagues (see p. 831) have been studying stem cell division in the Drosophila testis, which contains both germline stem cells (GSCs) and somatic cyst stem cells (CySCs). GSCs divide asymmetrically by maintaining a fixed cell polarity within the stem cell niche. Now, the researchers use time-lapse live imaging to show that CySC asymmetric division involves the repositioning of a randomly located mitotic spindle during or near anaphase onset. Spindle repositioning, they report, requires functional centrosomes, the motor protein Dynein and the actin-membrane linker Moesin, and is required to achieve the high-fidelity asymmetric CySC divisions that maintain both GSC and CySC numbers. The researchers speculate that the use of multiple mitotic schemes may be a general mechanism whereby divisions of different stem cell populations are coordinated in complex tissues.

Eyeing up neuronal circuits

The Drosophila optic lobe shares many characteristics with mammalian visual systems and might provide a powerful model for investigating the formation of visual processing circuits. Little is known, however, about the mechanisms that create neuronal diversity and organise neuronal circuits in the medulla, the optic lobe’s primary region. Now, on p. 983, Makoto Sato and colleagues describe the key features of the developing fly medulla. They show that, during larval development, the medulla is subdivided into concentric zones that are characterised by the expression of the transcription factors Drifter, Runt, Homothorax and Brain-specific homeobox. The birth order of the medulla neurons correlates with the expression pattern of these factors, they report, and each neuronal type exhibits an extensive but defined pattern of migration that disrupts the concentric zones during early pupal development. These results, and those of clonal analyses, lead the researchers to suggest that the concentric zone genes may form a genetic hierarchy that specifies neuronal identity and establishes neuronal circuits in the developing medulla.

Marking up germline imprints

Genomic imprinting – epigenetic modifications that ensure that certain genes are expressed from only one of the two inherited chromosomes – is crucial for normal development. Mammalian imprinted genes are associated with differentially methylated regions (DMRs) that are CpG methylated on one parental chromosome. At least 21 DMRs become methylated in the mouse germline and, on p. 811, Hiroyuki Sasaki and co-workers analyse a panel of these gametic DMRs. The extent of methylation of these DMRs differs significantly from that of embryonic DMRs, they report, suggesting that gametic DMRs should be used to identify the features that establish imprinting in the germline. They also show that maternal gametic DMRs appear as unmethylated islands in male germ cells, and unexpectedly identify widespread oocyte-specific non-CpG methylation. Finally, they report that DMR methylation changes dynamically during early development, indicating that DMRs are not fully protected from preimplantation epigenetic reprogramming. These results underscore the importance of using gametic DMR sequences for the study of imprint establishment.

Also…

PAR proteins are conserved regulators of cell polarity, and recent studies, reviewed here by Jeremy Nance and Jennifer Zallen, have identified elaborate links between PAR proteins and cytoskeletal proteins that help set-up molecular asymmetries and hence establish polarity within a cell. See the Review on p. 799

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MBL Embryology Course

Posted by , on 8 February 2011

Images taken by students in the 2010 MBL Embryology Course

Dear students, postdocs and mentors,

We write to share our enthusiasm about the MBL Embryology course and to encourage graduate students and postdoctoral fellows to apply for the 2011 summer course “Embryology: Concepts and Techniques in Modern Developmental Biology” at the Marine Biological Laboratory from June 5 – July 17, 2011.  The application deadline has now been extended, and the MBL will accept applications up to Feb. 15th (although the website will continue to give a Feb 1 deadline).  Further course description and application information is available at

http://www.mbl.edu/education/courses/summer/course_embryo.html

This course provides a unique intensive laboratory-lecture experience in contemporary developmental biology.  Students receive instruction from leaders in the field and also have the opportunity to conduct a series of laboratory exercises/investigations using state-of-the-art equipment and a wide range of model and non-model developmental organisms.  We believe that the unique educational experience provided by the Embryology Course is not available at any home institution.  In our experience, students leave this course with an increased breadth of understanding together with practical and novel laboratory experiences and a greatly expanded network of scientific colleagues.

The curriculum is divided into three areas: 1) modern comparative embryology and molecular phylogeny, cell lineage and cell specification; 2) pattern and organ formation; and 3) transcriptional regulation and the analysis of gene networks and developmental pathways.  Students will be exposed to a broad variety of marine and terrestrial invertebrates and vertebrates, and the increasingly sophisticated methods employed to analyze their development. Daily lectures, extended discussions and frequent informal talks provide an intense intellectual experience where students and faculty alike are immersed in sophisticated and continuously changing conceptual and experimental explorations.

We assure you that funds are available to provide substantial financial assistance to defray the cost of tuition.  In 2010 the MBL was able to provide up to 75% of these costs from NIH funding to the course as well as from endowed scholarships.  We expect to provide similar financial aid in 2011.

From our experience as faculty in the course and now as the co-directors, it is our belief that sending a student to this course is a proven, sound investment for the scientific future of the student, lab, and the developmental biology community, and requires only a relatively short absence from the home institution.

If you have any questions please contact Lee, Nipam or Carol Hamel, Admissions Coordinator, at admissions@mbl.edu

Sincerely,

Nipam Patel

University of California, Berkeley

nipam@uclink.berkeley.edu

Lee Niswander

University of Colorado Denver

Lee.Niswander@ucdenver.edu

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JSDB meeting

Posted by , on 8 February 2011

There’s still time to register for this years JSDB meeting. The deadline for abstract submission has been extended until February 10th.

JSDB meetings have been held almost entirely in English in recent years and not only offer an exciting scientific program, but also a chance to discover Japan.  This year the conference will be held in Okinawa, the largest of the subtropical Ryukyu islands which form the southernmost tip of the Japanese archipelago. Okinawan culture is unique; even if you have visited Japan before, Okinawa offers something different and is well worth a trip.

Check out the JSDB homepage for more information.

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Reflections on Natural History

Posted by , on 7 February 2011


One of the highlights of working at RIKEN CDB is undoubtedly the arrival upon my desk of “Library News”. Within this publication lies the eclectic column written by institute deputy director Shigeru Kuratani. These bimonthly articles are lively and often illuminating insights into the field of evolutionary morphology, frequently embracing topics such as art, literature, philosophy, and architecture.

There is plenty to entertain developmental biologists, including reviews of several classic anatomy texts such as De Beer’s “The Development of the Vertebrate Skull” and Ramón y Cajal’s “Histology of the Nervous System of Man and Vertebrates”. The pursuit of rare texts and prints is a common theme in many issues and a real sense of enthusiasm for science, history, and adventure is evident as Dr. Kuratani details his quests for classic anatomical text books throughout his career, for treasured natural history plates from the antiquarian markets on the banks of the Seine, and for particular rare specimens of moths resident in the mountains of Japan.

An enlightening and entertaining way to pass time over a cup of coffee, these library columns are now available from the Kuratani lab website (http://www.cdb.riken.jp/emo/clm.html).

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Natural Disasters and University Disruptions

Posted by , on 6 February 2011

Natural disasters can be powerfully destructive forces. At the very least, they have a habit of interrupting our lives and work. Damage varies depending on the intensity of nature’s fury and how prepared a city (or institution) is for a particular emergency. This can also influence how challenging recovery will be, in the aftermath.

The University Queensland was fortunate in many ways after the Southern Queensland floods, during which 3/4 of the state was submerged. Its St. Lucia campus lay next to the Brisbane River, but it only experienced low-level flooding, and so a handful of buildings were affected. Most escaped damaged. Partly this came from a lesson learned in 1974, the last time the university had experienced intense flooding (levels of up to 6.7 meters. this time water levels rose to about 4-5 meters). Since then, new buildings were predominantly established on higher ground. Post flooding, clean up crews were able to clear the debris and the university re-opened within days.

About 3 weeks later, Cyclone Yasi, category 5 (highest level there is, with gale force winds of up to 285 km/hr) hit Northern Queensland. Major cities in that region include Cairns and Townsville. The damage has been extensive according to recent news reports, with uproot trees, property damage, beached boats etc. Now, thousands are currently without power.  However, as cities were well prepared and properly evacuated, the death toll remains at one.

(Images from Flickr CC, by robandstephaustralia)

James Cook University (JCU), world renown for environmental research, closed its campuses at Townsville and Cairns on the morning of Feb. 2 in anticipation of the cyclone. Over 12 hours later, Yasi hit in the wee hours of Feb. 3. Clean up has been taking place, with the university set to re-open its campuses on Monday, Feb. 7. Many universities, like JCU, has a list of emergency procedures to take, in the event of a disaster or other threats to campus and students. It has a website informing staff and students on how the university responds.

This includes appointing an emergency controller who will  relay messages to staff, arrange any special measures for protecting equipment etc. Another page lists off how to ensure personal safety. As cyclones affect Queensland every year, it’s recommended steps can be quite detailed. i.e. During a storm, it may be necessary to shut off power and wear hardy clothing.

In a previous post on UQ and the Flood, Pablo Astudillo commented that Chile’s universities experienced an Earthquake, 8.8 on the richter scale (last year in Feb. 2010), followed by a tsunami and possibly some fires. Perhaps the only thing invariably worse than one natural disaster, is two or several in a row.

So, for any of you reading this, what kind of natural disruptions have you experienced? And how has this affected your research? Click here for a short survey.

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EuroStemCell: connecting scientists with European citizens

Posted by , on 3 February 2011

I’m one of a team of science communicators, scientists, clinicians and social scientists involved in a project called EuroStemCell. It’s an EU-funded project that unites more than 90 European stem cell and regenerative medicine research laboratories in a coordinated effort to engage with the public about our science, and support others to do the same. We’ve got lots going on – this post gives you an introduction to what we’re all about, and we’ll keep you updated as the project unfolds. (more…)

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the Node image competition

Posted by , on 3 February 2011

[updated 24/2] – New deadline: March 15

To celebrate the successful first half year of the Node, we’re running a competition.

A Node
Latin, Nodus – a knot
In general – a point of intersection
In developmental biology – an embryonic tissue that
patterns a developing embryo

All you have to do is send us an image (it can be, for example, a photo, drawing or microscopic image) related to:
(a) developmental biology; and
(b) some sort of intersection.
Make sure to include a brief description of the image, and only send in your own work.

Think about it carefully, and think out of the box.

Here are a few ideas to get you started….
Two developmental biologists in a knot (well – it’s an intersection of sorts…)
The intersection of two points in development
The intersection of ideas of developmental significance

Email your image to thenode@biologists.com before February 28 March 15 (new deadline!), noon GMT

In March, we will post the top 3 images on the Node, and then everyone will be able to vote for their favourite. Don’t worry if you want to stay anonymous – we don’t have to put your name up on display – just the picture that you send us!

The winner will get to commission their own TipArt work, worth $50 (US dollars), to prominently display in their lab or at home. TipArt is a website celebrating creativity at the lab bench with artwork made of pipette tips.

Terms and Conditions are available here
Competition Rules are available here
Closing date is February 28th March 15 2011 (12:00GMT)

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Meeting report from the 2010 Cold Spring Harbor Asia Conference “Molecular Switches and Genome Function in Stem Cells and Development”

Posted by , on 3 February 2011

In 2010 Cold Spring Harbor Laboratories building upon the success of its educational programs established an equivalent program in Asia and Pacific Rim centered in Suzhou, China – Cold Spring Harbor Conferences Asia (CSHCA). This development echoes the spectacular advances in biological research throughout the region (especially in China) over the past 30 years. The program includes large conferences, training workshops and small-scale, by-invitation meetings covering a broad spectrum of biomedical research topics as well as other fields of modern biology. It is planned that in near future the Conference Center will be supplemented by research facilities thereby creating an Asian research hub styled on the famous CSHL.

The Conference which took place on 21-25 September 2010 gathered more than 100 participants all over the world. It was set up in the new campus combining throughout ultramodern convenience and world-class architectural and landscape design beside Dushu Lake of Suzhou. Situated quite afar from the Suzhou downtown, the venue imposed tranquility suitable for consequential exchange of scientific ideas and fruitful discussions.

The central theme of the meeting was the iPS cell technology. So the Plenary Lecture delivered by Andras Nagy (Mount Sinai Hospital, Toronto) was dedicated to a closer look at the somatic cell reprogramming and consequences of the process for the stability of genome. It seems that the price we have to pay for our ability to turn almost every cell into the pluripotent one is the danger of inadvertent genomic aberrations which happen even after the retrovirus-free reprogramming. This might have quite strong implications for any therapeutic use of iPS cells in future. Nevertheless, the attempts to use iPSC for medical purposes were reported by researchers from Duanqing Pei’s lab (Guangzhou Institutes of Biomedicine and Health, GIBH). One  application was the modeling of human syndromes in human iPSC for test the gene therapy approaches and screening chemical compounds with the potential to correct an abnormality (in collaboration with Miguel Esteban, GIBH, and Axel Schambach, Hannover Medical School). Pentao Liu (Wellcome Trust Sanger Institute, Cambridge, UK) reported his lab’s work on identification of two additional genetic factors which dramatically improve and shorten the reprogramming process when used with four Yamanaka factors. Interesting evolutionary aspect of Sox2 function in pluripotent cell was demonstrated by Hitoshi Niwa (CDB, RIKEN Kobe); he suggested that a new function of the critical transcription factor may arise in evolution without structural changes in the molecule.

Many oral presentations were dedicated also to various adult stem cell systems, and the talk of Nick Barker (Hubrecht Institute, Utrecht) on intestinal crypt stem cells was in the focus of the meeting’s interest. In addition to revealing the key role of Lrg5 (Tcf/β-catenin target) in maintaining self-renewal of intestinal stem cells, he demonstrated an intriguing aspect of stem cell function – competition of stem cells within their niche. Quite a surprise, probably for many participants, was the presentation of Richard P. Harvey (Victor Chang Cardiac Research Institute, Australia) about the presence of multipotent stem cells (CFU-Fs) in adult mammalian heart. George C. Yeoh (University of Western Australia) addressed the recurrent and controversial issue of liver stem cells, describing inflammation-induced LPC, liver progenitor cells, which rapidly proliferate in vitro, survive repeated cycles of freezing/thawing and capable to differentiate into at least two types of liver cells: hepatocytes and cholangiocytes. Toshio Suda (Keio University, Tokyo) elaborated further on his theme of the hypoxic niche for hematopoietic stem cells (HSCs). It turns out that HSCs require a precise regulation of HIF-1α levels in order to maintain their quiescence in adult bone marrow. Interesting findings on the role of hemogenic endothelium in the ontogenesis of HSCs were presented by members of Shin-Ichi Nishikawa laboratory (CDB, RIKEN Kobe).

Practically all other oral presentations communicated the results of very impressive research. Among them most memorable were the addressing the role of stem cells in prostate cancer by Michael Shen (Columbia University Medical Center, New York), and latest insights on germ cell specification in vivo and in vitro (Mitinori Saitou, Graduate School of Medicine, Kyoto University).

Coffee breaks and lobby talks (sometimes with local beer tasting) proved to be exceptionally productive for friendly discussions, deeper insight into the presented works and, perhaps, for carrier opportunities for young Chinese researchers. Well, since the Chinese Ministry of Science and Technology has been reported to have established the National Key Program on stem cells (with large funding of corresponding research) in 2010, some foreign scientists may ponder the idea to move to China and set up their research there.

The Conference culminated in visiting the famous Lingering Garden of Suzhou, a UNESCO World Heritage Site. Artist performances, classical Chinese singing and dancing added a historical dimension to the vigor and intellectual strength of modern China.

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EMBO Workshop. Frontiers in Sensory Development, Barcelona, Spain

Posted by , on 2 February 2011

by MorBCN Flickr creative commons

Barcelona is the setting for the EMBO Workshop, Frontiers in Sensory Development from 3rd-6th May, 2011. The meeting will focus on different aspects of sensory development, function and evolution in both vertebrate and invertebrate systems. We hope this workshop will allow a better understanding of common themes in sensory function and will encourage colleagues working in different systems to exchange and discuss ideas and techniques. The schedule will feature invited talks, selected oral talks, poster sessions, and many opportunities to socialize in Barcelona.

The meeting will take place in at the PRBB Institute, located on the seafront of the Mediterranean Sea.

To register visit here (abstract submission is soon)

The flyer can be downloaded here

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The (re)birth of the DSDB

Posted by , on 1 February 2011

As the world of research into developmental biology becomes larger, and the arrival of online communities such as The Node allows us to bring that world a little closer to hand, the importance of using scientific communities to share expertise and experience only grows.   Therefore, here in the Netherlands we are pleased to announce that a little over a week ago the Hubrecht Institute in Utrecht hosted the inaugural meeting of the recently reformed Dutch Society for Developmental Biology (DSDB).

Upon coming to the Netherlands as a postdoc over a year ago, I was a little surprised there was no active developmental biology society or community in place, particularly considering that research which was being conducted in the Netherlands in the early 1900’s was one of the early initiatives for the founding of the first Society for Developmental biology (more about the new society later, first it’s time for a brief trip through history…).

Born in 1853, Ambrosius Hubrecht (for whom the modern Hubrecht Institute is named) was Professor of Zoology at Utrecht University.  He amassed a vast collection of embryological material, and his fascination for Darwin’s evolutionary theory led him into correspondence with Darwin himself.  In 1911, Hubrecht founded the ‘Institut Internationale d’Embryologie’ (IIE), a selective society of embryologists who would meet and discuss aspects of comparative embryology.  The home of the IIE, where meetings would take place, was Hubrecht’s private home in the centre of Utrecht.

A year after Hubrecht’s death in 1915, it was decided to establish the first Hubrecht Laboratory at Hubrecht’s house in Utrecht, and Daniel de Lange became the first director, leading the IIE, and  continuing to organise small international meetings between 1930 and 1938.  At this time, the IIE existed to serve the scientific needs of others, in the field of descriptive comparative embryology.
Concurrently, the field of experimental embryology was making great strides, and in 1968 the IIE renamed itself as the International Society of Developmental Biologists (ISDB), retaining its function as a discussion forum, and keeping its headquarters at the Hubrecht Laboratory

In Europe, and for some time, the functions of the ISDB were assumed in parallel by the European Developmental Biology Organisation (EDBO), grouping together the European national societies of Developmental Biology. At the time this included the Dutch NVOB (Netherlands Society for Developmental Biology). In 1997 the ISDB took over all EDBO functions, and became the world umbrella of national societies of developmental biology.  At this point, the NVOB lost its momentum (but was never officially dissolved), while the ISDB has continued to increase its affiliated members, as the international development community continues to grow.

Therefore, the large community of developmental biologists we belong to came about in part through the activities of a similar society formed here in the Netherlands 100 years ago.  It seemed a shame that a country with a rich history in developmental biology research and with much exciting research still taking place here, had lost its roots somewhat.  After an initial meeting of interested scientists in the summer last year, the DSDB/NVOB has been reborn.

The first meeting was a 1 day event, with 15 speakers (mostly PI’s from within the Netherlands) covering topics including axis patterning, developmental clocks, cell migration, organogenesis, hematopoiesis, plant growth and flowering and small RNAs .  The full program can be found on the DSDB website.  Discussion afterwards yielded the conclusion that the day had been a great success, and that there is definitely the need and enthusiasm for the resurrection of such a community in the Netherlands.

This initial meeting served to familiarise all developmental groups in the Netherlands with the research topics that are the main point of focus in different labs. In future years I would like to see the expansion of the meeting, hopefully so that it can also provide a forum for younger scientists to showcase their own work.  The mission statement of the society is to serve as a forum for developmental biologists in the Netherlands and, through the ISDB, throughout the world.  It should facilitate the sharing of conceptual and technical expertise within our field, and allow us to share research output and stimulate discussions through yearly meetings.  And of course, it will function as a national training network for young scientists. Certainly, as a young postdoc coming from a very interactive developmental biology community in England, my hope is that this society will grow and will once more flourish as a resource for developmental biologists in the Netherlands.  There is a website (it’s running but still rather under construction) for the new society, which can be found at www.nedvob.nl

The committee members for the new DSDB are:

Secretary: Dies Meijer (ErasmusMC, Rotterdam)

Treasurer: Rik Korswagen, (Hubrecht Institute, Utrecht)

President: Jacqueline Deschamps (Hubrecht Institute and UMC, Utrecht)

(Meeting co-organisers – Ben Scheres, Jeroen Bakkers, Susana Lopes and Derk ten Berge)

Membership to the society is now open, and membership enquiries can be directed to Rik Korswagen.

Many thanks to the organisers for getting the society up and running again, and to the NWO for financial support in organising the first meeting.  Also many thanks also to Jacqueline for a digested history of Dutch Dev Bio.



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