Background: One of the most important factors in breast cancer (BC) mortality is treatment delay. The primary goal of this survey was to identify factors affecting the total delay time (TDT) in Turkish BC patients. Methods: A total of 1031 patients with BC were surveyed using a uniform questionnaire. The time between discovering the first symptom and signing up for the first medical visit (patient delay time; PDT) and the time between the first medical visit and the start of therapy (system delay time; SDT) were modelled separately with multilevel regression. Results: The mean PDT, SDT and TDT were 4.8, 10.5 and 13.8 weeks, respectively. In all, 42% of the patients had a TDT >12 weeks. Longer PDT was significantly correlated with disregarding symptoms and having age of between 30 and 39 years. Shorter PDT was characteristic of patients who: had stronger self-examination habits, received more support from family and friends and had at least secondary education. Predictors of longer SDT included disregard of symptoms, distrust in success of therapy and medical system and having PDT in excess of 4 weeks. Shorter SDT was linked to the age of >60 years. Patients who were diagnosed during a periodic check-up or opportunistic mammography displayed shorter SDT compared with those who had symptomatic BC and their first medical examination was by a surgeon. Conclusion: TDT in Turkey is long and remains a major problem. Delays can be reduced by increasing BC awareness, implementing organized population-based screening programmes and founding cancer centres.
We present a case of a 40-year-old woman with small-cell carcinoma (SCC) of the rectum. She had profuse bleeding in rectum for 5 d. By colonoscopy, polyps were determined in the rectum and biopsies were carried out. Histopathologically, the polyps were adenomatous. Because of the profuse bleeding in rectum, she underwent low anterior resection. After the diagnosis of SCC, she received intravenous chemotherapy with standard doses of siklofosfamid, adriamycin, and vepesid. Nevertheless, intracranial metastases were revealed and she died 6 mo after the operation.
The objective of the present study was to investigate the effect of leptin on the
progression of colorectal carcinoma to metastatic disease by analyzing the serum
leptin concentration and Ob-R gene expression in colon cancer tissues. Tissue
samples were obtained from 31 patients who underwent surgical resection for
colon (18 cases) and metastatic colon (13 cases) cancer. Serum leptin
concentration was determined by an enzyme-linked immunosorbent assay (ELISA) and
Ob-R mRNA expression by real-time polymerase chain reaction (RT-PCR) for both
groups. ELISA data were analyzed by the Student t-test and
RT-PCR data were analyzed by the Mann-Whitney U-test. RT-PCR results
demonstrated that mRNA expression of Ob-R in human metastatic colorectal cancer
was higher than in local colorectal cancer tissues. On the other hand, mean
serum leptin concentration was significantly higher in local colorectal cancer
patients compared to patients with metastatic colorectal cancer. The results of
the present study suggest a role for leptin in the progression of colon cancer
to metastatic disease without weight loss. In other words, significantly
increased Ob-R mRNA expression and decreased serum leptin concentration in
patients with metastatic colon cancer indicate that sensitization to leptin
activity may be a major indicator of metastasis to the colon tissue and the
determination of leptin concentration and leptin gene expression may be used to
aid the diagnosis.
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