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Dive into the research topics where Katarina Kollar is active.

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Featured researches published by Katarina Kollar.


International Journal of Cell Biology | 2009

Molecular Mechanisms Involved in Mesenchymal Stem Cell Migration to the Site of Acute Myocardial Infarction

Katarina Kollar; Matthew M. Cook; Kerry Atkinson; Gary Brooke

Mesenchymal stem cells or multipotent mesenchymal stromal cells (both referred to as MSC) have been shown in some studies to have a beneficial effect on myocardial recovery after infarct. Current strategies for MSC delivery to heart involve intravenous, intraarterial, and intramuscular delivery. Different routes of MSC delivery and a lack of knowledge of the mechanisms that MSC utilise to migrate in vivo has most likely led to the marked variations in results that have been found. This review aims to summarise the current knowledge of MSC migratory mechanisms and looks to future methods of MSC manipulation prior to delivery in order to enhance MSC migration and engraftment.


International Journal of Cell Biology | 2009

Cellular Therapy for Repair of Cardiac Damage after Acute Myocardial Infarction

Matthew M. Cook; Katarina Kollar; Gary Brooke; Kerry Atkinson

Cardiovascular diseases, particularly acute myocardial infarction, are the leading causes of death worldwide. Important advances have been made in the secondary treatment for cardiovascular diseases such as heart transplantation and medical and surgical therapies. Although these therapies alleviate symptoms, and may even improve survival, none can reverse the disease process and directly repair the lasting damage. Thus, the cure of cardiovascular diseases remains a major unmet medical need. Recently, cellular therapy has been proposed as a candidate treatment for this. Many stem and progenitor cell populations have each been suggested as a potential basis for such therapy. This review assesses some of the more notable exogenous adult cell candidates and provides insights into the mechanisms by which they may mediate improvement in cardiac function following acute myocardial infarction. Research into the cellular therapy field is of great importance for the further planning of clinical trials for cardiac cellular myoplasty.


Genomics data | 2015

Multipotent human stromal cells isolated from cord blood, term placenta and adult bone marrow show distinct differences in gene expression pattern.

Nicholas Matigian; Gary Brooke; Faten Zaibak; Tony Rossetti; Katarina Kollar; Rebecca Pelekanos; Celena Heazlewood; Alan Mackay-Sim; Christine A. Wells; Kerry Atkinson

Multipotent mesenchymal stromal cells derived from human placenta (pMSCs), and unrestricted somatic stem cells (USSCs) derived from cord blood share many properties with human bone marrow-derived mesenchymal stromal cells (bmMSCs) and are currently in clinical trials for a wide range of clinical settings. Here we present gene expression profiles of human cord blood-derived unrestricted somatic stem cells (USSCs), human placental-derived mesenchymal stem cells (hpMSCs), and human bone marrow-derived mesenchymal stromal cells (bmMSCs), all derived from four different donors. The microarray data are available on the ArrayExpress database (www.ebi.ac.uk/arrayexpress) under accession number E-TABM-880. Additionally, the data has been integrated into a public portal, www.stemformatics.org. Our data provide a resource for understanding the differences in MSCs derived from different tissues.


Hamostaseologie | 2011

Therapeutic potential of intravenously administered human mesenchymal stromal cells

Katarina Kollar; E. Seifried; R. Henschler

Mesenchymal stem cells (MSC) represent a stem and progenitor cell population that has been shown to promote tissue recovery in pre-clinical and clinical studies. The study of MSC migration following systemic infusion of exogenous MSC is difficult. The challenges facing these efforts are due to a number of factors, including defining culture conditions for MSC, the phenotype of cultured MSC, the differences observed between cultured MSC and freshly isolated MSC. However, even if, MSC populations consist of a mixture of stem and more committed multipotent progenitors, it remains probable that these cell populations are still useful in the clinic as discussed in this review.


Journal of Clinical Medicine | 2013

Engraftment Outcomes after HPC Co-Culture with Mesenchymal Stromal Cells and Osteoblasts

Matthew M. Cook; Michael R. Doran; Katarina Kollar; Valerie Barbier; Ingrid G. Winkler; Jean-Pierre Levesque; Gary Brooke; Kerry Atkinson

Haematopoietic stem cell (HSC) transplantation is an established cell-based therapy for a number of haematological diseases. To enhance this therapy, there is considerable interest in expanding HSCs in artificial niches prior to transplantation. This study compared murine HSC expansion supported through co-culture on monolayers of either undifferentiated mesenchymal stromal cells (MSCs) or osteoblasts. Sorted Lineage− Sca-1+ c-kit+ (LSK) haematopoietic stem/progenitor cells (HPC) demonstrated proliferative capacity on both stromal monolayers with the greatest expansion of LSK shown in cultures supported by osteoblast monolayers. After transplantation, both types of bulk-expanded cultures were capable of engrafting and repopulating lethally irradiated primary and secondary murine recipients. LSKs co-cultured on MSCs showed comparable, but not superior, reconstitution ability to that of freshly isolated LSKs. Surprisingly, however, osteoblast co-cultured LSKs showed significantly poorer haematopoietic reconstitution compared to LSKs co-cultured on MSCs, likely due to a delay in short-term reconstitution. We demonstrated that stromal monolayers can be used to maintain, but not expand, functional HSCs without a need for additional haematopoietic growth factors. We also demonstrated that despite apparently superior in vitro performance, co-injection of bulk cultures of osteoblasts and LSKs in vivo was detrimental to recipient survival and should be avoided in translation to clinical practice.


Stem Cells | 2014

Identification and characterization of circulating variants of CXCL12 from human plasma: effects on chemotaxis and mobilization of hematopoietic stem and progenitor cells.

R. Richter; A. Jochheim-Richter; F. Ciuculescu; Katarina Kollar; E. Seifried; U. Forssmann; Dennis Verzijl; Martine J. Smit; Xavier Blanchet; P. von Hundelshausen; Christian Weber; W.G. Forssmann; R. Henschler


Faculty of Health | 2015

Multipotent human stromal cells isolated from cord blood, term placenta and adult bone marrow show distinct differences in gene expression pattern

Nicholas Matigian; Gary Brooke; Faten Zaibak; Tony Rossetti; Katarina Kollar; Rebecca Pelekanos; Celena Heazlewood; Alan Mackay-Sim; Christine A. Wells; Kerry Atkinson


Faculty of Health; Institute of Health and Biomedical Innovation | 2013

Engraftment outcomes after HPC co-culture with mesenchymal stromal cells and osteoblasts

Matthew M. Cook; Michael R. Doran; Katarina Kollar; Valerie Barbier; Ingrid G. Winkler; Jean-Pierre Levesque; Gary Brooke; Kerry Atkinson


Science & Engineering Faculty | 2010

Mesenchymal stromal cells transiently alter the inflammatory milieu post-transplant to delay graft-versus-host disease

Melinda E. Christensen; Brie E. Turner; Laura J. Sinfield; Katarina Kollar; Hannah Cullup; Nigel J. Waterhouse; Derek N. J. Hart; Kerry Atkinson; Alison M. Rice


Archive | 2010

The molecular mechanisms utilised by mesenchymal stem cells in migration to acute myocardial infarction

Katarina Kollar

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Kerry Atkinson

University of Queensland

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Gary Brooke

University of Queensland

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Matthew M. Cook

Queensland University of Technology

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Faten Zaibak

University of Melbourne

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Michael R. Doran

Queensland University of Technology

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