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8 research outputs found

Strongly correlated quantum dots in weak confinement potentials and magnetic fields

Author: A. Karlhede
A.H. MacDonald
A.V. Filinov
C. de C. Chamon
C. Yannouleas
C.G. Darwin
D. Pfannkuche
E. Abrahams
F. Selva
J.J. Palacios
K. Hirose
L. Kouwenhoven
L.P. Kouwenhoven
M. Koskinen
M.-C. Cha
Min-Chul Cha
O. Klein
P. Hawrylak
P.A. Maksym
R. Egger
S. Siljamaki
S. Tarucha
S. Tarucha
S.-R. Eric Yang
S.-R. Eric Yang
S.-R. Eric Yang
S.A. Mikhailov
S.A. Mikhailov
S.M. Reimann
T.H. Oosterkamp
V. Fock
Publication venue: 'American Physical Society (APS)'
Publication date: 03/03/2003
Field of study

We explore a strongly correlated quantum dot in the presence of a weak confinement potential and a weak magnetic field. Our exact diagonalization studies show that the groundstate property of such a quantum dot is rather sensitive to the magnetic field and the strength of the confinement potential. We have determined rich phase diagrams of these quantum dots. Some experimental consequences of the obtained phase diagrams are discussed.Comment: 5 pages, 7 figures, new and updated figure

arXiv.org e-Print Archive

Crossref

Expression of claudin-11 by tumor cells in cutaneous squamous cell carcinoma is dependent on the activity of p38δ

Author: Farshchian M
Kahari VM
Kallajoki M
Kivisaari A
Nissinen L
Peltonen J
Peltonen S
Piipponen M
Raiko L
Riihila P
Siljamaki E
Publication venue: 'Wiley'
Publication date: 28/10/2022
Field of study

The incidence of cutaneous squamous cell carcinoma (cSCC) is rapidly increasing, and the prognosis of patients with metastatic disease is poor. There is an emerging need to identify molecular markers for predicting aggressive behaviour of cSCC. Here, we have examined the role of tight junction (TJ) components in the progression of cSCC. The expression pattern of mRNAs for TJ components was determined with RNA sequencing and oligonucleotide array-based expression analysis from cSCC cell lines (n=8) and normal human epidermal keratinocytes (NHEK, n=5). The expression of CLDN11 was specifically elevated in primary cSCC cell lines (n=5), but low or absent in metastatic cSCC cell lines (n=3) and NHEKs. Claudin-11 was detected in cell-cell contacts of primary cSCC cells in culture by indirect immunofluorescence analysis. Analysis of a large panel of tissue samples from sporadic UV-induced cSCC (n=65), cSCC in situ (n=56), actinic keratoses (n=31), seborrhoeic keratoses (n=7) and normal skin (n=16) by immunohistochemistry showed specific staining for claudin-11 in intercellular junctions of keratinizing tumor cells in well and moderately differentiated cSCCs, whereas no staining for claudin-11 was detected in poorly differentiated tumors. The expression of claudin-11 in cSCC cells was dependent on the activity of p38 delta MAPK and knock-down of claudin-11 enhanced cSCC cell invasion. These findings provide evidence for the role of claudin-11 in regulation of cSCC invasion and suggest loss of claudin-11 expression in tumor cells as a biomarker for advanced stage of cSCC

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