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Molecular studies of irradiation and SN-38 on colorectal cancer / Åsa Wallin.

Wallin, Åsa, 1976- (författare)
Alternativt namn: Wallin, Molecular studies of irradiation and SN-38 on colorectal cancer / Åsa Wallin Linköping : Linköping University, 1976-
Sun, Xiao-Feng (preses)
Svanvik, Joar, 1942- (preses)
Naredi, Peter, 1955- (opponent)
Linköpings universitet. Institutionen för klinisk och experimentell medicin (utgivare)
Alternativt namn: Linköping University. Department of Clinical and Experimental Medicine
Alternativt namn: Linköping University. Faculty of Health Sciences. Department of Clinical and Experimental Medicine
Alternativt namn: IKE
Hälsouniversitetet i Östergötland (utgivare)
Alternativt namn: Linköpings högskola. Medicinska fakulteten
Alternativt namn: Linköpings universitet. Medicinska fakulteten
Alternativt namn: Linköping University. Faculty of Health Sciences
Alternativt namn: Linköping University. Health University
Alternativt namn: Hälsouniversitetet i Linköping
Se även: Universitetet i Linköping. Medicinska fakulteten (tidigare namn)
Publicerad: Linköping : Linköping University, Department of Clinical and Experimental Medicine, 2008
Engelska 1 onlineresurs (60 sidor)
Serie: Linköping University medical dissertations, 0345-0082 ; 1070
Läs hela texten (Sammanfattning och ramberättelse från Linköping University Electronic Press)
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  • E-bokAvhandling(Diss. (sammanfattning) Linköping : Linköpings universitet, 2008)
Sammanfattning Ämnesord
Stäng  
  • Colorectal cancer (CRC) is one of most common cancer diseases worldwide. In Sweden approximately 5,000 new cases of CRC are generated each year, which makes it the third most common cancer disease among both men and women. The past decades of improved treatment strategies have considerably increased the five-year survival for CRCpatients. However more could be achieved in this area, in particular for metastatic CRC,which is the cause of most CRC-related deaths. Therefore it is important to study the biological response to certain treatments induced in CRC to find valuable predictiveand/or prognostic factors to select patients for better suited treatments. The aim of this thesis was to gain insight into the molecular changes that occur following irradiation or treatment with SN-38 in rectal cancer patients or colon cancercell lines by studying the RNA expression, protein expression, DNA cell cycledistribution and apoptotic response. The expression of phosphatase of regenerating liver(PRL) proteins was investigated in rectal cancers from 125 patients included in arandomized clinical trial of preoperative radiotherapy (RT). Increased expression of PRLswas seen at the invasive margin of primary and metastatic cancers compared with theinner area of the tumors. Moreover, strong PRL staining at the invasive margin correlatedto distant recurrence and worse survival of patients in the RT group but not in non-RTgroup (Paper I). Radiosensitivity was studied by treating KM12C, KM12SM andKM12L4a colon cancer cell lines with radiation. KM12C is of low metastatic naturecompared with the highly metastatic KM12SM and KM12L4a. Upregulation of ΔNp73and PRL-3 might contribute to the radioresistant phenotype in KM12C. In contrast,KM12L4a shows a high frequency of apoptosis and lack of upregulation of ΔNp73, PRL-3 and survivin, which might explain its radiosensitive phenotype (Paper II). KM12C,KM12SM and KM12L4a were treated with SN-38 which inhibits topoisomerase 1 (topo-1). The results show that SN-38 induces G2/S arrest and possess the capacity to triggerapoptosis in the three cell lines (Paper III). To further elucidate SN-38 effect on these celllines, the gene expression profile following SN-38 treatment was studied. Oligonucleotidearrays consisting of ~27,000 spots were hybridized with sample and reference cDNA.Both unsupervised and supervised hierarchical clustering analysis, and functional analysiswere performed. Supervised hierarchical clustering gives a strong signal of 1453discriminated genes, the vast majority being upregulated. Both upregulated anddownregulated genes point toward a favorable impact of SN-38 regarding the apoptoticpathways. For example RhoB and Bax are upregulated together with downregulation ofKras and survivin, which promotes apoptosis (Paper IV). In conclusion, PRLs may be valuable biomarkers for RT resistance, predicting apoor prognosis in rectal cancer patients. Targeting radio-resistance factors, such asΔNp73 and survivin may contribute to an increased sensitivity to RT. SN-38 affects cellproliferation and apoptosis. 

Ämnesord

Medical and Health Sciences  (ssif)
Clinical Medicine  (ssif)
Cancer and Oncology  (ssif)
Medicin och hälsovetenskap  (ssif)
Klinisk medicin  (ssif)
Cancer och onkologi  (ssif)
MEDICINE  (svep)
Surgery  (svep)
Oncology  (svep)
MEDICIN  (svep)
Kirurgi  (svep)
Onkologi  (svep)
Tarmcancer  -- behandling (sao)

Genre

government publication  (marcgt)

Indexterm och SAB-rubrik

Colorectal cancer (CRC)
Molecular changes
SN-38
Vej Matsmältningsorganen (medicinsk gastroenterologi)
Vep Onkologi (läran om tumörer)

Klassifikation

616.994347 (DDC)
Vej (kssb/8)
Vep (kssb/8)
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