Identification of aberrantly regulated genes in diseased skin using the cDNA differential display technique

被引：60

作者：

Rivas, MV

Jarvis, ED

Morisaki, S

Carbonaro, H

Gottlieb, AB

Krueger, JG

机构：

[1] ROCKEFELLER UNIV, INVEST DERMATOL LAB, NEW YORK, NY 10021 USA

[2] ROCKEFELLER UNIV, LAB ANIM BEHAV, NEW YORK, NY 10021 USA

[3] UMDNJ, ROBERT WOOD JOHNSON MED SCH, NEW BRUNSWICK, NJ USA

来源：

JOURNAL OF INVESTIGATIVE DERMATOLOGY | 1997年 / 108卷 / 02期

关键词：

connexin-26; squamous cell carcinoma antigen; gap junctions; serine protease inhibitor; mitochondrial NADH5 and 6;

D O I：

10.1111/1523-1747.ep12334217

中图分类号：

R75 [皮肤病学与性病学];

学科分类号：

100206 ;

摘要：

It is hypothesized that psoriasis may be caused by aberrant gene expression, In an effort to identify and clone psoriasis-specific genes, we compared gene expression in normal, tape-stripped (wounded), and psoriatic skin using the cDNA differential display technique, Four genes not previously described in psoriasis-connexin 26, a gap junction protein; squamous cell carcinoma antigen-l (SCCA1), a serine protease inhibitor; and mitochondrial NAD subunits 5 and 6-were identified as having very high expression levels in psoriatic skin, II situ hybridizations showed that connexin 26 mRNA was expressed 10-fold higher in psoriatic and 4-fold higher in tape-stripped epidermis than in controls, SCCA1. showed a 40-fold increase in mRNA expression, whereas mitochondrial NAD5 and NAD6 expression was increased 10- and 20-fold, respectively, in psoriatic skin, Northern blots confirmed the increased expression of connexin 26, SCCA1, and NAD6 genes in psoriatic skin, Immunohistochemistry showed that connexin 26 protein was strongly expressed in spinous keratinocytes from psoriatic skin and chronic wounds, but was absent in normal epidermis, These studies demonstrate the usefulness of this approach for identifying genes that are conditionally expressed in growth-activated human skin.

引用

页码：188 / 194

页数：7

共 38 条

[1] ALTSCHUL SF, 1990, J MOL BIOL, V215, P403, DOI 10.1006/jmbi.1990.9999
[2] SEQUENCE AND ORGANIZATION OF THE HUMAN MITOCHONDRIAL GENOME
ANDERSON, S
BANKIER, AT
BARRELL, BG
DEBRUIJN, MHL
COULSON, AR
DROUIN, J
EPERON, IC
NIERLICH, DP
ROE, BA
SANGER, F
SCHREIER, PH
SMITH, AJH
STADEN, R
YOUNG, IG
[J]. NATURE, 1981, 290 (5806) : 457 - 465
[3] PLASMA-MEMBRANES IN PSORIATIC CELLS - FREEZE-FRACTURE STUDY
CAPUTO, R
INNOCENTI, M
GASPARINI, G
PELUCHETTI, D
[J]. JOURNAL OF INVESTIGATIVE DERMATOLOGY, 1978, 71 (04) : 245 - 249
[4] A 2-DIMENSIONAL GEL PROTEIN DATABASE OF NONCULTURED TOTAL NORMAL HUMAN EPIDERMAL-KERATINOCYTES - IDENTIFICATION OF PROTEINS STRONGLY UP-REGULATED IN PSORIATIC EPIDERMIS
CELIS, JE
CRUGER, D
KIIL, J
DEJGAARD, K
LAURIDSEN, JB
RATZ, GP
BASSE, B
CELIS, A
RASMUSSEN, HH
BAUW, G
VANDEKERCKHOVE, J
[J]. ELECTROPHORESIS, 1990, 11 (03) : 242 - 254
[5] SINGLE-STEP METHOD OF RNA ISOLATION BY ACID GUANIDINIUM THIOCYANATE PHENOL CHLOROFORM EXTRACTION
CHOMCZYNSKI, P
SACCHI, N
[J]. ANALYTICAL BIOCHEMISTRY, 1987, 162 (01) : 156 - 159
[6] URF6, LAST UNIDENTIFIED READING FRAME OF HUMAN MTDNA, CODES FOR AN NADH DEHYDROGENASE SUBUNIT
CHOMYN, A
CLEETER, MWJ
RAGAN, CI
RILEY, M
DOOLITTLE, RF
ATTARDI, G
[J]. SCIENCE, 1986, 234 (4776) : 614 - 618
[7] 6 UNIDENTIFIED READING FRAMES OF HUMAN MITOCHONDRIAL-DNA ENCODE COMPONENTS OF THE RESPIRATORY-CHAIN NADH DEHYDROGENASE
CHOMYN, A
MARIOTTINI, P
CLEETER, MWJ
RAGAN, CI
MATSUNOYAGI, A
HATEFI, Y
DOOLITTLE, RF
ATTARDI, G
[J]. NATURE, 1985, 314 (6012) : 592 - 597
[8] PROBES FOR RARE MESSENGER-RNAS REVEAL DISTRIBUTED CELL SUBSETS IN CANARY BRAIN
CLAYTON, DF
HUECAS, ME
SINCLAIRTHOMPSON, EY
NASTIUK, KL
NOTTEBOHM, F
[J]. NEURON, 1988, 1 (03) : 249 - 261
[9] COOPER KD, 1990, DERMATOL CLIN, V8, P737
[10] GROWTH-FACTOR AND PROTOONCOGENE EXPRESSION IN PSORIASIS
ELDER, JT
KLEIN, SB
TAVAKKOL, A
FISHER, GJ
NICKOLOFF, BJ
VOORHEES, JJ
[J]. JOURNAL OF INVESTIGATIVE DERMATOLOGY, 1990, 95 (05) : S7 - S9

← 1 2 3 4 →