scholarly journals Risk Of Cancer And Radiation Dose Received By Patients From Common Diagnostic Radiological Examinations

2019 ◽  
Vol 13 (1) ◽  
pp. 66-69
Author(s):  
Ridha Jawad Al-Basri

Background: Although radiological diagnostic studies (RDS) are an important and acceptable part of medical practice, it is not without hazards. It is associated with increased risk of cancer. Unfortunately the typical and safe dose of each radiological examination is not known. Most of our knowledge of cancer risk comes from studies of survivors of those exposed to whole body radiation from atomic bomb in Hiroshima & Nagasaki, jobs associated with radiation exposure, Chernobyl survivors & patients treated with radiation therapy for cancer and other diseases.  Objectives   To estimate radiation dose received by patients from diagnostic radiological examinations and lifetime attributable risk of cancer (LTARC). Type of the study: A prospective study.  Methods   A prospective study was conducted in Al-Kindi Teaching Hospital (KTH) during the period from 1st June to 31st august 2016. The study was performed on 910 adult patients. There were 595 males (65.38%) and 315 females (34.62%); mean age was 41.5 years (range 20-63).Different RDS were considered including chest-x ray (CXR), skull x-ray(SXR),    x-ray of limbs and pelvis (LPXR) for orthopedic causes , computed tomography scan (CTS) and mammography (MG) . Results   CXR was performed for 260 (28.57%) patients which delivers 0.12 mSv. SXR was done for 160 (17.58%) patients which delivers 0.3 mSv. LPXR was performed for 220 (24.175%) which delivers 0.3-0.6 mSv. MG exposes 150 (16.48%) to 3 mSv. While CTS ,which         delivers 6.2-16 mSv according to anatomic area being scanned, was done for 120(13.19%) patients.  Conclusion    There is great abuse for using RDS from both patients and doctors, without realizing their danger and association with cancer development. It was proved that RDS expos patients to different kinds of tissues injury including cancer.

Blood ◽  
2012 ◽  
Vol 120 (21) ◽  
pp. 2913-2913
Author(s):  
Francesco Spina ◽  
Paolo Potepan ◽  
Giovanna Trecate ◽  
Eros Montin ◽  
Vittorio Montefusco ◽  
...  

Abstract Abstract 2913 Introduction: Standard assessment of bone disease in multiple myeloma (MM) is based on skeletal X-ray (XR) and magnetic resonance (MR) of the spine (MRS). Diffusion-weighted MR (DW-MR) is a novel functional MR that detects changes of water diffusion through cells in tissues. To assess the value of DW-MR to detect bone lesions in MM, we designed a prospective study comparing whole-body DW-MR with XR and MRS. The study included symptomatic patients (pts) at diagnosis or at relapse before the start of the treatment; they performed XR, MRS, conventional whole-body MR (WB-MR), and whole-body DW-MR at enrolment (time point 1, T1), after treatment (T2), and after 6 months of follow-up (T3). Clinical and hematologic, including bone marrow (BM), disease evaluations were done at the same time points. The study was approved by the Institutional Review Board in 2008 (protocol 44/08). Methods: The primary objective was to assess whether DW-MR could detect more focal lesions (FL) than XR and MRS. Secondary objectives were to correlate the changes of FL detected by DW-RM with response, to assess the prognostic value of DW-RM, and to compare DW-MR with WB-MR. MRS, WB-MR and DW-MR were done in a single 45-minute session on a standard 1.5 Tesla MR scanner. DW-MR consisted of multiple stacked axial Echo Planar Imaging sequences at 4 b-values, evaluated by PET-like Maximum Intensity Projection and Multi-Planar reconstructions at the highest b-value (1000). Each exam was independently read by 3 radiologists experienced in MM. 53 bone segments per exam were evaluated in whole-body imaging (XR, WB-MR and DW-MR); 25 segments were evaluated in spine imaging (MRS and DW-MR). All the patterns (focal, diffuse, mixed, and salt-and-pepper) of bone lesions were recorded. Matching FL detected by >=2 radiologists were counted for the present analysis. Statistics were carried out with the Wilcoxon signed rank test for methods comparisons and the Kruskal-Wallis test to assess intra-patient changes through the time points. Survival and relapse were analyzed by Kaplan-Meier and Cumulative Incidence method with log-rank and Gray's tests. All tests were 2-sided. Results: Between 2008 and 2010, 36 symptomatic pts were enrolled: 43% were at diagnosis, 57% at relapse; 71% of pts had ISS stage 1 MM. The most frequent isotype was IgG (57%), median BM infiltration was 30%. FISH on selected CD138+ plasma cells detected t(4;14) and del(17) in 9 and 6% of pts. At T1, the DW-MR detected more FL than standard XR (306 vs 117 FL, p<0.01), WB-MR (306 vs 225 FL, p=0.02), and MRS (165 vs 116 FL, trend, p=0.08). At T2, a similar number of FL was detected by DW-MR and XR (97 vs 104 FL, p=0.99) and MRS (20 vs 20 FL, p=1.00); DW-MR detected more FL than WB-MR (97 vs 60 FL, p=0.01). At T3, the DW-MR detected more FL than WB-MR (88 vs 45 FL, p<0.01) and MRS (24 vs 11 FL, p=0.05), and similar FL compared to XR (88 vs 62 FL, p=0.27). Considering all the time points, the DW-MR detected more FL than XR (p=0.01), WB-MR (p<0.01) and MRS (p=0.02). Between T1 and T2, all pts were treated with IMIDS or bortezomib–based regimens, 33% underwent a stem cell transplant. Overall response rate (ORR) was 73%. DW-MR detected significant changes of FL according to disease response at T2 (from 79 to 15 FL in >=VGPR, from 69 to 27 in PR, and from 34 to 55 FL in SD or PD, p=0.04 [whole body]; p=0.02 [spine]). Also MRS consistently detected response (p=0.04), whereas WB-MR showed only a weak correlation (p=0.13); XR did not detect response (p=0.55). Between T2 and T3, pts had minor changes of disease status (72% ORR), and, accordingly, all the radiological exams did not show significant changes in FL. One-, 2- and 3-year progression-free survival (PFS) was 80, 62 and 37% (median, 30 months), OS was 88, 79 and 76% (median not reached), and relapse incidence was 15, 32, and 54% (median, 21 months). Since the median number of FL detected by DW-MR at T1 was 4 (range, 0–49 FL), we compared PFS, relapse, and OS by the presence of <=4 FL or >4 FL before treatment. Patients with <=4 FL at DW-MR had better PFS (72 vs 50% at 2 years, p=0.02) and less relapse incidence (17 vs 50%, p<0.01) than those with >4 FL, whereas OS was not different (84 vs 75%, p=0.76). Conclusions: DW-MR is superior to XR, MRS, and WB-MR in detecting FL in MM. The number of FL detected by DW-MR before treatment predicts PFS and relapse incidence. DW-MR is a functional imaging that effectively detects the bone disease changes according to treatment response and can be used to monitor disease response. Disclosures: No relevant conflicts of interest to declare.


Oral Oncology ◽  
2021 ◽  
Vol 116 ◽  
pp. 105240
Author(s):  
Sebastian Zschaeck ◽  
Julian Weingärtner ◽  
Pirus Ghadjar ◽  
Peter Wust ◽  
Felix Mehrhof ◽  
...  

2021 ◽  
Vol 21 ◽  
pp. S115
Author(s):  
Michael Gundesen ◽  
Jon Thor Asmussen ◽  
Einar Haukås ◽  
Michael Schubert ◽  
Niels Abildgaard ◽  
...  

2003 ◽  
Vol 98 ◽  
pp. S299
Author(s):  
Virender K. Sharma ◽  
Mankanwal S. Sachdev ◽  
Jonathan A. Leighton ◽  
Russell I. Heigh ◽  
Janice A. Post ◽  
...  

PEDIATRICS ◽  
1977 ◽  
Vol 60 (5) ◽  
pp. 669-672
Author(s):  
Shashikant M. Sane ◽  
Robert A. Worsing ◽  
Cornelius W. Wiens ◽  
Rajiv K. Sharma

To assess the value of routine preoperative chest x-ray films in pediatric patients, a prospective study of 1,500 patients, ages newborn to 19 years, was undertaken. Of all the patients, 7.5% demonstrated at least one roentgenographic abnormality, with 4.7% of the patients demonstrating a totally unsuspected significant roentgenographic anomaly. In 3.8% of the patients, surgery was either postponed or cancelled or the anesthetic technique was altered as a result of the roentgenographic finding. It is believed that the routine preoperative chest film is justified if the film is evaluated before surgery and the results clinically followed up.


PEDIATRICS ◽  
1978 ◽  
Vol 61 (2) ◽  
pp. 332-333
Author(s):  
Henry M. Feder

McCarthy et al. in their article "Temperature Greater Than or Equal to 40 C in Children Less Than 24 Months of Age: A Prospective Study" (Pediatrics 59:663, May 1977) recommend using both WBC count (≥ 15,000/cu mm) and ESR (≥ 30 mm/hr) for screening febrile young children for pneumonia or bacteremia. If either is elevated they suggest doing blood cultures and taking a chest roentgenogram. However, in 25% of their patients with bacteremia and 42% of their patients with pneumonia neither WBC count nor ESR was elevated, leaving a sizable false-negative group.


2019 ◽  
Vol 477 (8) ◽  
pp. 1879-1888 ◽  
Author(s):  
Andrew D. Sobel ◽  
Adam E.M. Eltorai ◽  
Barrett Weiss ◽  
P. Kaveh Mansuripur ◽  
Arnold-Peter C. Weiss

2020 ◽  
Vol 9 (8) ◽  
pp. 2659 ◽  
Author(s):  
Sapir Anani ◽  
Gal Goldhaber ◽  
Adi Brom ◽  
Nir Lasman ◽  
Natia Turpashvili ◽  
...  

Background: Frailty and sarcopenia are associated with frequent hospitalizations and poor clinical outcomes in geriatric patients. Ascertaining this association for younger patients hospitalized in internal medicine departments could help better prognosticate patients in the realm of internal medicine. Methods: During a 1-year prospective study in an internal medicine department, we evaluated patients upon admission for sarcopenia and frailty. We used the FRAIL questionnaire, blood alanine-amino transferase (ALT) activity, and mid-arm muscle circumference (MAMC) measurements. Results: We recruited 980 consecutive patients upon hospital admission (median age 72 years (IQR 65–79); 56.8% males). According to the FRAIL questionnaire, 106 (10.8%) patients were robust, 368 (37.5%) pre-frail, and 506 (51.7%) were frail. The median ALT value was 19IU/L (IQR 14–28). The median MAMC value was 27.8 (IQR 25.7–30.2). Patients with low ALT activity level (<17IU/L) were frailer according to their FRAIL score (3 (IQR 2–4) vs. 2 (IQR 1–3); p < 0.001). Higher MAMC values were associated with higher ALT activity, both representing robustness. The rate of 30 days readmission in the whole cohort was 17.4%. Frail patients, according to the FRAIL score (FS), had a higher risk for 30 days readmission (for FS > 2, HR = 1.99; 95CI = 1.29–3.08; p = 0.002). Frail patients, according to low ALT activity, also had a significantly higher risk for 30 days readmission (HR = 2.22; 95CI = 1.26–3.91; p = 0.006). After excluding patients whose length of stay (LOS) was ≥10 days, 252 (27.5%) stayed in-hospital for 4 days or longer. Frail patients according to FS had a higher risk for LOS ≥4 days (for FS > 2, HR = 1.87; 95CI = 1.39–2.52; p < 0.001). Frail patients, according to low ALT activity, were also at higher risk for LOS ≥4 days (HR = 1.87; 95CI = 1.39–2.52; p < 0.001). MAMC values were not correlated with patients’ LOS or risk for re-admission. Conclusion: Frailty and sarcopenia upon admission to internal medicine departments are associated with longer hospitalization and increased risk for re-admission.


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