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1 ates with disease duration and the degree of spongiosis.
2 C) is depleted, in parallel with reversal of spongiosis.
3 ut not early, even in regions with prominent spongiosis.
4 eptor 2-mediated pruritus and MyD88-mediated spongiosis.
5 ive deposits, astrocytosis, myelin loss, and spongiosis.
6 d brainstem dissemination also induced acute spongiosis.
8 ative scoring of neuronal loss, gliosis, and spongiosis and immunocytochemical and ultrastructural ch
9 psoriasiform acanthosis in association with spongiosis and infiltration of both the epidermis and de
12 , CJD mice had the hallmark features of CJD, spongiosis and proteinase K-resistant PrP aggregates, in
13 d epidermal barrier, microbial colonization, spongiosis, and eosinophil infiltration, but also aspect
14 Histologically, scattered glial nodules, spongiosis, and mineralization were found in the basal g
16 on accompanied by progressive neuronal loss, spongiosis, and neurite degeneration in the cerebellum.
17 concentrated in regions of the brain rich in spongiosis, and the magnitude of responses was similar t
18 L-4 and IL-13, we found coal tar to diminish spongiosis, apoptosis, and CCL26 expression, all AD hall
19 mi-quantitative histopathological scoring of spongiosis, astrocytosis and prion protein deposition.
23 eratinocytes is the main cause of eczema and spongiosis in patients with the common inflammatory skin
25 ost closely resembled AD hallmarks including spongiosis, more severe keratinocyte differentiation def
26 lysis showed marked epidermal acanthosis and spongiosis, neovascularization, and elevated number of i
27 of circumscribed neuronal loss, gliosis, and spongiosis of limbic neocortical areas and frontal, temp
30 n cortical magnetization transfer ratios and spongiosis (P = 0.02), but not prion protein deposition
31 levant signaling pathways that contribute to spongiosis, proliferation, generation of proinflammatory
33 hese studies revealed that acute MLV-induced spongiosis results from two separable activities of Env.
35 um in its central portion, exhibiting marked spongiosis, vascular proliferation, and a chronic inflam