DcR2 (TRAIL-R4) siRNA and adenovirus delivery of TRAIL (Ad5hTRAIL) break down in vitro tumorigenic potential of prostate carcinoma cells

Şanlioğlu, Ahter Dilşad; Karaçay, Bahri; Koksal, Ismail Turker; Griffith, Thomas S.; Şanlıoğlu, Salih

doi:10.1038/sj.cgt.7701087

Cited by 40 publications

(31 citation statements)

References 39 publications

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“…37,38 Most of them use recombinant adenoviruses or lentiviruses, 39,40 but because of the possibility of recombination with wildtype adenovirus and the antiviral immune response, these approaches have been limited to research use. 41 More recently, electroporation has been applied in vivo and shown to be potentially safe for clinical use.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of tumor growth and induction of apoptosis in prostate cancer cell lines by overexpression of tissue inhibitor of matrix metalloproteinase-3

Zhang

Zhao

et al. 2009

Cancer Gene Ther

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The destruction of extracellular matrix by matrix metalloproteinases is a key event in cancer progression. The tissue inhibitors of metalloproteinases can restrain tumor growth by inhibiting these enzymes. We sought to determine whether overexpression of tissue inhibitor of metalloproteinase-3 (TIMP-3) could suppress the malignant phenotype of human prostate cancer cell line PC-3M. Stable overexpression of TIMP-3 inhibited cell proliferation significantly by MTT assay. Both early and late apoptosis were observed in TIMP-3 overexpressing cells, and flow cytometry analysis showed S-phase blocking of the cell cycle. Monolayer invasion assay and transwell invasion assay showed significantly decreased invasive potential in TIMP-3 overexpressing cells compared with control cells. Cell adhesion and motility were also lower after TIMP-3 was overexpressed. In vivo, cells stably overexpressing TIMP-3 completely lost the ability to form tumors after injection into nude mice. Transfection of TIMP-3 into established tumors by electroporation also had a significant antitumor effect. TIMP-3-treated tumor tissues had significant apoptosis by TUNEL assay. These results showed that overexpression of TIMP-3 inhibits invasion and proliferation of prostate cancer cells in vitro and inhibits tumor growth in vivo. The experiments suggest a potential use for TIMP-3 in the gene therapy of prostate cancer.

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Section: Discussionmentioning

confidence: 99%

Inhibition of tumor growth and induction of apoptosis in prostate cancer cell lines by overexpression of tissue inhibitor of matrix metalloproteinase-3

Zhang

Zhao

et al. 2009

Cancer Gene Ther

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“…6,7 TRAIL-induced cell death can be specifically inhibited by two membrane-bound antagonistic receptors, TRAIL-R3 (DcR1, LIT or TRID) or TRAIL-R4 (DcR2 or TRUNDD). 2 These receptors have been shown to be expressed and to prevent TRAIL-induced cell death in various human primary tumor cells, including lymphomas, lung, breast and prostate carcinomas, [8][9][10] but the inhibitory potential of this receptor still remains controversial. 11 Although TRAIL-R3 is a GPI-anchored receptor that sequesters TRAIL into lipid rafts, TRAIL-R4 interacts with TRAIL-R2 within the DISC, and impairs caspase-8 processing, 12 thus, inhibiting TRAILinduced apoptosis.…”

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confidence: 99%

Chemotherapy overcomes TRAIL-R4-mediated TRAIL resistance at the DISC level

et al. 2010

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“…Apopto sis is ini ti a ted when the se re cep tors are en ga ged by the ir li gands, that is, Fas li gand, TNF, and TRA -IL, res pec ti vely, which are eit her fre e in the cir cula ti on or bo und to the mem bra ne of cyto to xic ef fec tor cells. [17][18][19][20] Nuc le ar fac tor-kap pa B (NF-kB) ac ti va ti on, in ad di ti on to an in cre a se in the mRNA le vels of TNF-a, TNFR1, cas pa se 8, and cas pa se 3, has be en do cu men ted in rat mo dels of re nal obstruc ti on.…”

Section: Discussionmentioning

confidence: 99%

Beneficial Effect of Doxazosin on Renal Apoptosis After Partial Bladder Outlet Obstruction

Kutlu¹,

Yalçinkaya²,

Elpek³

et al. 2010

Turkiye Klinikleri J Med Sci

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A AB BS S T TR RA AC CT T O Ob b j je ec c t ti i v ve e: : It is not known whet her in hi bi ti on of α1-ad re no re cep tor in a rat mo del of par ti al blad der out let obs truc ti on (BO O) ca u ses dec re a se in tu bu lar and glo me ru lar cell de ath by apop to sis and pre ven ti on of sub se qu ent inf lam ma ti on and fib ro sis. The aim of this study was to demons tra te the re la ti ons hip bet we en apop to sis and do xa zo si n   α1-ad re no cep tor an ta go nist) in rat kid neys da ma ged by par ti al BO O. M Ma a t te e r ri i a al l a an nd d M Me et t h ho od ds s: : A to tal of 45 adult fe ma le Wis tar rats,with a me an weight of 250 g we re ran domly al lo ca ted to four ex pe ri men tal gro ups as: sham-ope ra ted rats (10 rats), sham-ope ra ted rats tre a ted with do xa zo sin (10 rats), par ti al BO O gro up (14 rats), and parti al BO O gro up tre a ted with do xa zo sin (11 rats). Par ti al BO O was sur gi cally in du ced. De tec ti on of cell apop to sis was do ne by TU NEL as say. R Re e s su ul lt ts s: : This in ves ti ga ti on re ve a led in cre a sed apop to sis in both tu bu lar and glo me ru lar cells of rats with par ti al BO O. Furt her mo re, the re sults of this study de mons tra ted that do xa zo sin tre at ment of rats re du ced apop to sis in tu bu lar and glo me ru lar cells in both the con trols and the rats with par ti al BO O. C Co on nc c l lu u s si i o on n: : We be li e ve that our observation of dec re a sed apop to sis in both tu bu lar and glo me ru lar cells of rats with par ti al BO O might be use ful to ga in new in sight in to the the ra pe u tic ef fect of do xa zo sin.K Ke ey y W Wo or rd ds s: : Apoptosis; kidney; doxazosin Ö ÖZ ZE ET T A Am ma aç ç: : Me sa ne çı kış obs trük si yo nu (MÇO) oluş tu ru lan sı çan mo de lin de α1 ad re no re sep tör in hi bis yo nu nun apo pi to zis ile tü bü ler ve glo me rü ler hüc re ölü mü ne yol açıp aç ma dı ğı ve son rasın da ge li şen inf la mas yon ve fib ro zi si en gel le yip en gel le me di ği bi lin me mek te dir. Do la yı sıy la, bu ça -lış ma nın ama cı kıs mi MÇO ile ha sar lan dı rıl mış sı çan böb rek le rin de apo pi to zis ile dok sa zo sin (al fa 1 re sep tör an ta go nis ti) ara sın da ki iliş ki yi gös ter mek tir. G Ge e r re eç ç v ve e Y Yö ön n t te em m l le er r: : Or ta la ma 250 gram ağır lı ğın da ki top lam 45 adet di şi Wis tar sı çan la rı 4 de ney sel gru ba ran do mi ze edil di: sham ope rasyon lu sı çan lar (10 sı çan), dok sa zo sin ile te da vi edi len sham ope ras yon lu sı çan lar (14 sı çan), kıs mi MÇO gru bu (14 sı çan), ve dok sa zo sin ile te da vi edi len kıs mi MÇO gru bu. Sı çan lar da ki kıs mi MÇO cer ra hi ola rak in dük len di. Hüc re apo pi to zi si TU NEL ana li zi tes pit edil di. B Bu ul l g gu u l la ar r: : Bu araş tır ma kıs mi MÇO' lu sı çan lar da hem tü bü ler hem de glo me rü ler hüc re ler de art mış apo pi to zi si gös ter miş -tir. Ay rı ca, bu ça lış ma nın so nuç la rı dok sa zo si nin kıs mi MÇO' lu sı çan lar da ve kon trol gru bu nu oluş-tu ran sı ça...

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DcR2 (TRAIL-R4) siRNA and adenovirus delivery of TRAIL (Ad5hTRAIL) break down in vitro tumorigenic potential of prostate carcinoma cells

Cited by 40 publications

References 39 publications

Inhibition of tumor growth and induction of apoptosis in prostate cancer cell lines by overexpression of tissue inhibitor of matrix metalloproteinase-3

Inhibition of tumor growth and induction of apoptosis in prostate cancer cell lines by overexpression of tissue inhibitor of matrix metalloproteinase-3

Chemotherapy overcomes TRAIL-R4-mediated TRAIL resistance at the DISC level

Beneficial Effect of Doxazosin on Renal Apoptosis After Partial Bladder Outlet Obstruction

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