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Home › Dataset Library › Data from a time course study of gene expression in a mouse model of osteoarthritis

Dataset: Data from a time course study of gene expression in a mouse model of osteoarthritis

The purpose of this study was to characterize the histologic development of OA in a mouse model where OA is induced by destabilization of...

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The purpose of this study was to characterize the histologic development of OA in a mouse model where OA is induced by destabilization of the medial meniscus (DMM model) and to identify genes regulated during different stages of the disease, using RNA isolated from the joint “organ” and analyzed using microarrays.427 genes from the microarrays passed consistency and significance filters. There was an initial up-regulation at 2 and 4 weeks of genes involved in morphogenesis, differentiation, and development, including growth factor and matrix genes, as well as transcription factors including Atf2, Creb3l1, and Erg. Most genes were off or down-regulated at 8 weeks with the most highly down-regulated genes involved in cell division and the cytoskeleton. Gene expression increased at 16 weeks, in particular extracellular matrix genes including Prelp, Col3a1 and fibromodulin.The results support a phasic development of OA with early matrix remodelling and transcriptional activity followed by a more quiescent period that is not maintained. A group of 9 mice was used for collection of RNA at time 0 (before surgery) when the animals were 12 weeks old. For the other time points, 9 DMM and 9 sham controls were sacrificed at 2, 4, 8, and 16 weeks after surgery for RNA isolation. The tissue included tibial plateau and femoral condyle articular cartilage, subchondral bone with any osteophytes, meniscus, and the joint capsule with synovium was used for RNA isolation. The tissue was treated with RNAlater® (Invitrogen) prior to freezing and storage at -800 C. RNA was extracted by homogenization using the Precellys 24 tissue homogenizer (Bertin Technologies purchased from MO BIO) and the amount and quality of the RNA was determined using an Agilent 2100 Bioanalyzer. RNA was pooled prior to microarray analysis such that 3 randomly selected samples from each surgical group and time point were pooled to create each biological replicate. Because 9 mice were used for each experimental group, a total of three biological replicates per group were analyzed using the Affymetrix Mouse Genome 430 2.0 oligonucleotide arrays as described. One replicate pool, which was from week two DMM mice, did not meet the RNA integrity level needed for microarray analysis; thus, this pool was not analyzed further, leaving two pools for the week two DMM mice.

Species:
mouse

Samples:
26

Source:
E-GEOD-41342

Updated:
Dec.12, 2014

Registered:
Nov.12, 2014


Factors: (via ArrayExpress)
Sample AGE PROTOCOL TIME POST-PROTOCOL
GSM1015207 12 weeks no surgery baseline
GSM1015207 12 weeks no surgery baseline
GSM1015207 12 weeks no surgery baseline
GSM1015210 14 weeks sham control surgery 2 weeks
GSM1015210 14 weeks sham control surgery 2 weeks
GSM1015210 14 weeks sham control surgery 2 weeks
GSM1015213 16 weeks sham control surgery 4 weeks
GSM1015213 16 weeks sham control surgery 4 weeks
GSM1015213 16 weeks sham control surgery 4 weeks
GSM1015216 20 weeks sham control surgery 8 weeks
GSM1015216 20 weeks sham control surgery 8 weeks
GSM1015216 20 weeks sham control surgery 8 weeks
GSM1015219 28 weeks sham control surgery 16 weeks
GSM1015219 28 weeks sham control surgery 16 weeks
GSM1015219 28 weeks sham control surgery 16 weeks
GSM1015222 14 weeks DMM surgery 2 weeks
GSM1015222 14 weeks DMM surgery 2 weeks
GSM1015224 16 weeks DMM surgery 4 weeks
GSM1015224 16 weeks DMM surgery 4 weeks
GSM1015224 16 weeks DMM surgery 4 weeks
GSM1015227 20 weeks DMM surgery 8 weeks
GSM1015227 20 weeks DMM surgery 8 weeks
GSM1015227 20 weeks DMM surgery 8 weeks
GSM1015230 28 weeks DMM surgery 16 weeks
GSM1015230 28 weeks DMM surgery 16 weeks
GSM1015230 28 weeks DMM surgery 16 weeks

Tags

  • articular cartilage
  • bone
  • capsule
  • cell
  • condyle
  • cytoskeleton
  • disease
  • fibromodulin
  • genome
  • joint
  • medial
  • medial meniscus
  • point
  • tibial

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