T. Kobayashi scite author profile

Monoclonal antibodies against human Cu,Zn-superoxide dismutase (SOD) and Mn-SOD were used to stain frozen sections of normal and abnormal human skin. In normal human epidermis, the Cu,Zn-SOD antibody almost exclusively stained the basal cells. Mn-SOD antibody weakly stained the whole of the epidermis but more predominantly the basal cell layer. In psoriasis, Cu,Zn-SOD antibody mainly stained the basal cells of the lowest parts of the elongated rete ridges. Basal cells corresponding to the tip of the dermal papillae were weakly stained. Mn-SOD staining was considerably decreased in the psoriatic epidermis. In squamous cell carcinoma, staining with both Cu,Zn-SOD and Mn-SOD antibodies was decreased, and single cells positive for Cu,Zn-SOD were scattered throughout the tumour nests. In basal cell epithelioma, Cu,Zn-SOD staining was intense and diffusely distributed throughout the tumour nests, while Mn-SOD staining was absent.

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Development of a Thin-Wall Superconducting Magnet for the Positron Spectrometer in the MEG Experiment

Ootani

Odashima

Kimura

et al. 2004

IEEE Trans. Appl. Supercond.

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Abstract-A thin-wall superconducting magnet was developed for the positron spectrometer in the MEG experiment. The magnet is specially designed to provide a gradient magnetic field to achieve good features of the spectrometer such as constant projected bending radius for monochromatic positrons and much quicker sweep of positrons than in the conventional uniform solenoidal field, which allows a stable operation of the spectrometer in a high rate muon beam. A high-strength aluminum-stabilized conductor was developed so as to minimize the thickness of the coil between the target and photon detector. A pair of compensation coils is implemented in the magnet to cancel stray field around the photon detector to be placed closely to the magnet. Design of the magnet and results from the excitation tests to measure performance of the magnet will be presented here.

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Expression of p21 (WAF1/CIP1) protein in clinical thyroid tissues

Ito

Kobayashi²,

Takeda³

et al. 1996

Br J Cancer

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Summary p21 (WAF1/CIP1) protein expression in various thyroid tissues, including thyroid carcinoma, was studied by means of immunohistochemistry using anti-p21 monoclonal antibody. Normal follicles and hyperplasias rarely expressed p21, whereas immunohistochemically positive cells were also too rarely found in follicular adenomas to justify these cases being classified as positive. Twenty eight of the 93 carcinomas examined (30.1%), however, were positive for p21. Of the p21-positive cases, 80% of the undifferentiated and 28.6% of the poorly differentiated carcinomas showed lesions co-expressing p21 and p53. If diffuse immunoreactivity of p53 reflects the p53 mutation, our results indicate that p21 in these carcinomas can be induced by p53-independent as well as by p53-dependent pathways. On the other hand, well-differentiated carcinomas did not co-express these two proteins and it therefore remains unclear whether p53-independent or p53-dependent pathways are predominant in this type of carcinoma. The incidence of expression of p21 was very similar in undifferentiated (26.3%), poorly (28.0%) and well-differentiated carcinomas (32.7%), even though they are characterised by different degrees of malignancy. Furthermore, no correlation between p21 expression and either clinical parameters or patient's prognosis could be established. These results suggest that p21 is only marginally related to the characteristics of thyroid carcinoma and can play only an adjuvant role in regulating the progression of this carcinoma.

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Cathepsin B and D expression in squamous cell carcinoma

Kawada¹,

Hara²,

Kominami³

et al. 1996

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To elucidate involvement of proteinases in malignancy of keratinocytes, expression of cathepsin B, a cysteine proteinase, and cathepsin D, an aspartic proteinase, was ascertained in formalin-fixed paraffin-embedded specimens of normal skin, squamous cell carcinoma (SCC). Bowen's disease, seborrhoeic keratosis and basal cell carcinoma (BCC). Presence of procathepsin B and an intermediate form of cathepsin D was confirmed by Western blotting and enzyme activity analysis. Cathepsin B stained more intensely in SCC tumour cells than in normal epidermis; staining patterns were diffuse, granular or both. Diffuse and granular patterns (procathepsin B and mature enzyme, respectively) appeared in inner and outer parts of tumour islands, respectively. Five of 20 cases of Bowen's disease showed diffuse enhanced cathepsin B expression; 20 cases of seborrhoeic keratosis or BCC did not. Cathepsin D stained intensely in tumour cells of half the SCC cases. The staining manner and distribution of cathepsins B and D was similar in the cytoplasm of cancer cells. No enhanced staining of cathepsin D was seen in any cases of Bowen's disease, seborrhoeic keratosis, or BCC. Coexistence and localization of active mature forms of cathepsins B and D suggests that cooperation between the two enzymes may play an important part in invasion of SCC.

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T. Kobayashi

Biochemical Characterization and Biologic Actions of Two Toxins (D-l and D-2) from Clostridium difficile

Superoxide dismutase in psoriasis, squamous cell carcinoma and basal cell epithelioma: an immunohistochemical study

Development of a Thin-Wall Superconducting Magnet for the Positron Spectrometer in the MEG Experiment

Expression of p21 (WAF1/CIP1) protein in clinical thyroid tissues

Cathepsin B and D expression in squamous cell carcinoma

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