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However, advancement in deriving functional HSCs from human pluripotent stem cells has been slow.
However, advancement in deriving functional HSCs from human pluripotent stem cells has been slow.

Reconstituting blood in humans to be boon for individuals suffering from blood cancer, sickle-cell anaemia: Study

ANI | Updated: Jan 01, 2020 19:50 IST

Washington D.C. [USA], Jan 1 (ANI): Finding out effective ways to reconstitute blood in humans will prove to be a boon for individuals suffering from ailments such as blood cancer and sickle-cell anaemia, say researchers.
Reconstitution involves the transplantation and engraftment of blood stem cells (hematopoietic stem cells or HSCs) which upon being transfused into the recipient, trigger the production of all types of blood cells, including platelets, white and red blood cells.
In current clinical practice, this is carried out by infusing HSCs obtained from a matched donor who is immunologically compatible with the patient in need (allogeneic transplantation), or by the expansion of the patient's own HSCs in the lab, and then re-infusing them back into the patient (ex-vivo, autologous transplantation).
However, the utility of both routes is currently limited by a number of factors.
First, in the case of allogeneic transplantation, the scarcity of matched donors significantly increases the waiting time, which could be detrimental to the patient.
Second, the ex vivo expansion of HSCs, whether allogeneic or autologous, has been a challenging task, due to the limited proliferative potential these cells exhibit in culture. These limitations have raised the need for other sources of HSCs that would alleviate the need for matched donors and yield functional HSCs in large quantities.
In 2007, Prof Shinya Yamanaka and colleagues demonstrated that somatic cells, like skin fibroblasts, could be reprogrammed back to a cellular state that resembled human embryonic stem cells (hESCs), which are a group of cells found in the blastocyst-stage human embryo and contribute solely to the development of the human fetus during pregnancy.
The reprogrammed cells were termed, Induced Pluripotent Stem Cells (iPSCs). In addition to their developmental potential, human ESCs and iPS cells display unlimited proliferative potential in culture, which makes them an ideal source of cells for regenerative medicine in general and for hematopoietic differentiation to obtain possibly unlimited quantities of HSCs. Therefore, there has been a growing interest to harness the potential of these cells for treating blood disorders.
However, advancement in deriving functional HSCs from human pluripotent stem cells has been slow. This has been attributed to an incomplete understanding of the molecular mechanisms underlying normal hematopoiesis.
In this review, the authors discuss the latest efforts to generate HSCs capable of long-term engraftment and reconstitution of the blood system from human pluripotent stem cells. Stem cell research has witnessed milestone achievements in this area in the last couple of years, the significance of which is discussed and analyzed in detail.
The authors additionally discuss two highly important families of transcription factors in the context of hematopoiesis and hematopoietic differentiation, the Homeobox (HOX) and GATA proteins.
These are thought of as master regulators, in the sense of having numerous transcriptional targets, which upon activation, could elicit significant changes in cell identity. The authors hypothesize that precise temporal control of the levels of certain members of these families during hematopoietic differentiation could yield functional HSCs capable of long-term engraftment.
The authors conclude the review with a summary of future perspectives, in which they discuss how newly developed techniques, like the deactivated-Cas9 (dCas9) gene-expression control system, can be utilised during the course of hematopoietic differentiation of pluripotent stem cells for precise temporal control of the aforementioned master regulators to achieve functional HSCs. (ANI)