Monika Dohse scite author profile

The characterization of hepatic progenitor cells is of great scientific and clinical interest. Here we report that intravenous injection of adult bone marrow cells in the FAH(-/-) mouse, an animal model of tyrosinemia type I, rescued the mouse and restored the biochemical function of its liver. Moreover, within bone marrow, only rigorously purified hematopoietic stem cells gave rise to donor-derived hematopoietic and hepatic regeneration. This result seems to contradict the conventional assumptions of the germ layer origins of tissues such as the liver, and raises the question of whether the cells of the hematopoietic stem cell phenotype are pluripotent hematopoietic cells that retain the ability to transdifferentiate, or whether they are more primitive multipotent cells.

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Cleavage of RIPK1 by caspase-8 is crucial for limiting apoptosis and necroptosis

Newton¹,

Wickliffe²,

Dugger³

et al. 2019

Nature

373

291

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Seborrhoeic dermatitis andPityrosporum(Malassezia) folliculitis: characterization of inflammatory cells and mediators in the skin by immunohistochemistry

et al. 2001

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An increase in NK1+ and CD16+ cells in combination with complement activation indicates that an irritant non-immunogenic stimulation of the immune system is important. The result with the interleukins showed both an increase in the production of inflammatory interleukins as well as in the regulatory interleukins for both TH1 and TH2 cells. Similarities to the immune response described for Candida albicans infections indicate the role of Malassezia in the skin response in seborrhoeic dermatitis and Pityrosporum folliculitis.

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Human Neural Stem Cells Induce Functional Myelination in Mice with Severe Dysmyelination

et al. 2012

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Shiverer-immunodeficient (Shi-id) mice demonstrate defective myelination in the central nervous system (CNS) and significant ataxia by 2 to 3 weeks of life. Expanded, banked human neural stem cells (HuCNS-SCs) were transplanted into three sites in the brains of neonatal or juvenile Shi-id mice, which were asymptomatic or showed advanced hypomyelination, respectively. In both groups of mice, HuCNS-SCs engrafted and underwent preferential differentiation into oligodendrocytes. These oligodendrocytes generated compact myelin with normalized nodal organization, ultrastructure, and axon conduction velocities. Myelination was equivalent in neonatal and juvenile mice by quantitative histopathology and high-field ex vivo magnetic resonance imaging, which, through fractional anisotropy, revealed CNS myelination 5 to 7 weeks after HuCNS-SC transplantation. Transplanted HuCNS-SCs generated functional myelin in the CNS, even in animals with severe symptomatic hypomyelination, suggesting that this strategy may be useful for treating dysmyelinating diseases.

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Monika Dohse

Purified hematopoietic stem cells can differentiate into hepatocytes in vivo

Cleavage of RIPK1 by caspase-8 is crucial for limiting apoptosis and necroptosis

Seborrhoeic dermatitis andPityrosporum(Malassezia) folliculitis: characterization of inflammatory cells and mediators in the skin by immunohistochemistry

Human Neural Stem Cells Induce Functional Myelination in Mice with Severe Dysmyelination

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