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5 results on '"Kuure, S. (Satu)"'

1. Scanning transmission soft X-ray spectromicroscopy of mouse kidney and liver

Author

Mansikkala, T. (Tuomas), Ohigashi, T. (Takuji), Salo, M. H. (Miia H.), Hiltunen, A. E. (Anniina E.), Vuolteenaho, R. (Reetta), Sipilä, P. (Petra), Kuure, S. (Satu), Huttula, M. (Marko), Uusimaa, J. (Johanna), Hinttala, R. (Reetta), Miinalainen, I. (Ilkka), Kangas, S. (Salla), Patanen, M. (Minna), Mansikkala, T. (Tuomas), Ohigashi, T. (Takuji), Salo, M. H. (Miia H.), Hiltunen, A. E. (Anniina E.), Vuolteenaho, R. (Reetta), Sipilä, P. (Petra), Kuure, S. (Satu), Huttula, M. (Marko), Uusimaa, J. (Johanna), Hinttala, R. (Reetta), Miinalainen, I. (Ilkka), Kangas, S. (Salla), and Patanen, M. (Minna)

Abstract

Scanning transmission X-ray microscopy (STXM) in the soft X-ray range is well-suited to study ultrastructural features of mammalian soft tissues. Especially at the carbon 1s edge, the imaging contrast varies drastically across the edge due to rapid changes in the X-ray absorption cross-section of functional groups present in the tissue samples enabling label-free soft X-ray spectromicroscopic studies. We present STXM spectromicroscopic imaging of mouse kidney and liver tissues. We especially concentrate on ultrastructural abnormalities in genetically modified Slc17a5 mice. STXM is a promising technique to study storage diseases without chemical alteration due to staining agents, but sample preparation poses a challenge.

Published
2023

2. The Finnish genetic heritage in 2022:from diagnosis to translational research

Author

Uusimaa, J. (Johanna), Kettunen, J. (Johannes), Varilo, T. (Teppo), Järvelä, I. (Irma), Kallijärvi, J. (Jukka), Kääriäinen, H. (Helena), Laine, M. (Minna), Lapatto, R. (Risto), Myllynen, P. (Päivi), Niinikoski, H. (Harri), Rahikkala, E. (Elisa), Suomalainen, A. (Anu), Tikkanen, R. (Ritva), Tyynismaa, H. (Henna), Vieira, P. (Päivi), Zarybnicky, T. (Tomas), Sipilä, P. (Petra), Kuure, S. (Satu), Hinttala, R. (Reetta), Uusimaa, J. (Johanna), Kettunen, J. (Johannes), Varilo, T. (Teppo), Järvelä, I. (Irma), Kallijärvi, J. (Jukka), Kääriäinen, H. (Helena), Laine, M. (Minna), Lapatto, R. (Risto), Myllynen, P. (Päivi), Niinikoski, H. (Harri), Rahikkala, E. (Elisa), Suomalainen, A. (Anu), Tikkanen, R. (Ritva), Tyynismaa, H. (Henna), Vieira, P. (Päivi), Zarybnicky, T. (Tomas), Sipilä, P. (Petra), Kuure, S. (Satu), and Hinttala, R. (Reetta)

Abstract

Isolated populations have been valuable for the discovery of rare monogenic diseases and their causative genetic variants. Finnish disease heritage (FDH) is an example of a group of hereditary monogenic disorders caused by single major, usually autosomal-recessive, variants enriched in the population due to several past genetic drift events. Interestingly, distinct subpopulations have remained in Finland and have maintained their unique genetic repertoire. Thus, FDH diseases have persisted, facilitating vigorous research on the underlying molecular mechanisms and development of treatment options. This Review summarizes the current status of FDH, including the most recently discovered FDH disorders, and introduces a set of other recently identified diseases that share common features with the traditional FDH diseases. The Review also discusses a new era for population-based studies, which combine various forms of big data to identify novel genotype–phenotype associations behind more complex conditions, as exemplified here by the FinnGen project. In addition to the pathogenic variants with an unequivocal causative role in the disease phenotype, several risk alleles that correlate with certain phenotypic features have been identified among the Finns, further emphasizing the broad value of studying genetically isolated populations.

Published
2022

3. Modeling rare human disorders in mice:the Finnish disease heritage

Author

Zárybnický, T. (Tomáš), Heikkinen, A. (Anne), Kangas, S. M. (Salla M.), Karikoski, M. (Marika), Martínez-Nieto, G. A. (Guillermo Antonio), Salo, M. H. (Miia H.), Uusimaa, J. (Johanna), Vuolteenaho, R. (Reetta), Hinttala, R. (Reetta), Sipilä, P. (Petra), Kuure, S. (Satu), Zárybnický, T. (Tomáš), Heikkinen, A. (Anne), Kangas, S. M. (Salla M.), Karikoski, M. (Marika), Martínez-Nieto, G. A. (Guillermo Antonio), Salo, M. H. (Miia H.), Uusimaa, J. (Johanna), Vuolteenaho, R. (Reetta), Hinttala, R. (Reetta), Sipilä, P. (Petra), and Kuure, S. (Satu)

Abstract

The modification of genes in animal models has evidently and comprehensively improved our knowledge on proteins and signaling pathways in human physiology and pathology. In this review, we discuss almost 40 monogenic rare diseases that are enriched in the Finnish population and defined as the Finnish disease heritage (FDH). We will highlight how gene-modified mouse models have greatly facilitated the understanding of the pathological manifestations of these diseases and how some of the diseases still lack proper models. We urge the establishment of subsequent international consortiums to cooperatively plan and carry out future human disease modeling strategies. Detailed information on disease mechanisms brings along broader understanding of the molecular pathways they act along both parallel and transverse to the proteins affected in rare diseases, therefore also aiding understanding of common disease pathologies.

Published
2021

4. TT2020 meeting report on the 16th transgenic technology meeting

Author

Hinttala, R. (Reetta), Kuure, S. (Satu), Hinttala, R. (Reetta), and Kuure, S. (Satu)

Abstract

The 16th transgenic technology (TT) meeting of the International Society of Transgenic technology (ISTT) took place on October 26–29th 2020 and was quite unique as it was the first-ever virtual meeting in the history of ISTT events. Dr. Rebecca Haffner-Krausz at Weizmann Institute of Science, Israel, was the local organizer of the meeting, which attracted 756 registered participants from 32 different countries.

Published
2021

5. Dynamic MAPK/ERK activity sustains nephron progenitors through niche regulation and primes precursors for differentiation

Author

Ihermann-Hella, A. (Anneliis), Hirashima, T. (Tsuyoshi), Kupari, J. (Jussi), Kurtzeborn, K. (Kristen), Li, H. (Hao), Kwon, H. N. (Hyuk Nam), Cebrian, C. (Cristina), Soofi, A. (Abdul), Dapkunas, A. (Arvydas), Miinalainen, I. (Ilkka), Dressler, G. R. (Gregory R.), Matsuda, M. (Michiyuki), Kuure, S. (Satu), Ihermann-Hella, A. (Anneliis), Hirashima, T. (Tsuyoshi), Kupari, J. (Jussi), Kurtzeborn, K. (Kristen), Li, H. (Hao), Kwon, H. N. (Hyuk Nam), Cebrian, C. (Cristina), Soofi, A. (Abdul), Dapkunas, A. (Arvydas), Miinalainen, I. (Ilkka), Dressler, G. R. (Gregory R.), Matsuda, M. (Michiyuki), and Kuure, S. (Satu)

Abstract

Summary The in vivo niche and basic cellular properties of nephron progenitors are poorly described. Here we studied the cellular organization and function of the MAPK/ERK pathway in nephron progenitors. Live-imaging of ERK activity by a Förster resonance energy transfer biosensor revealed a dynamic activation pattern in progenitors, whereas differentiating precursors exhibited sustained activity. Genetic experiments demonstrate that MAPK/ERK activity controls the thickness, coherence, and integrity of the nephron progenitor niche. Molecularly, MAPK/ERK activity regulates niche organization and communication with extracellular matrix through PAX2 and ITGA8, and is needed for CITED1 expression denoting undifferentiated status. MAPK/ERK activation in nephron precursors propels differentiation by priming cells for distal and proximal fates induced by the Wnt and Notch pathways. Thus, our results demonstrate a mechanism through which MAPK/ERK activity controls both progenitor maintenance and differentiation by regulating a distinct set of targets, which maintain the biomechanical milieu of tissue-residing progenitors and prime precursors for nephrogenesis.

Published
2018

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