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"The obesity pandemic continues to increase on a world-wide basis with over 70% of the United States population being either overweight or obese. Hematologic malignancies have recently been identified among the obesity associated malignancies spanning the lifespan from childhood to the elderly and include leukemia, myeloma, lymphoma and others. In addition to the etiologic association between obesity and hematologic malignancies, the presence of obesity has profound effects on therapy by impacting pharmacokinetics of chemotherapeutic agents, dose, adipocyte metabolism and drug distribution. These may be particularly important in hematopoietic stem cell transplantation. Another important aspect of the association of obesity with hematologic malignancies is the increased incidence of obesity in children who successfully complete therapy for acute lymphoblastic leukemia. This and other observations indicate important relations between the hematopoietic systems and fat metabolism. This volume on Energy Balance in Hematologic Malignancies will provide an important volume in this series and a basis for better understanding etiology, mechanisms, therapeutics implications and experimental approaches. This volume of energy balance and cancer will focus on the relation of obesity to hematologic malignancies, the epidemiology, potential mechanisms, and thereapeutic considerations including effects on pharmacologic and physical approaches as well as the delayed effects of therapy on energy balance."
New York: Springer Science , 2012
e20420995
eBooks  Universitas Indonesia Library
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Indah Melati Suciyanie
"Latar Belakang: Identifikasi manusia yang hidup dan mati sangat penting dalam odontologi forensik. Beberapa prosedur untuk estimasi usia dewasa saat kematian yang banyak digunakan adalah metode morfohistologis, yaitu Tooth Cementum Annulation (TCA) dan Root Dentin Translucency (RDT). Namun, masih sedikit penelitian yang membandingkan kedua metode tersebut dan akurasinya dalam memperkirakan usia dewasa saat kematian. Tujuan: Untuk menguji dan membandingkan akurasi antara metode TCA dan RDT. Metode: Pencarian data dilakukan melalui lima database elektronik: Pubmed, SCOPUS, EBSCO, ScienceDirect, dan Wiley, dengan mengikuti pedoman dari Preferred Reporting Items for Systematic Review and Meta-Analyses (PRISMA). Hasil: Dari total 1178 studi, 28 studi diikutsertakan untuk analisis kualitatif dan 23 studi untuk meta-analisis. Metode RDT menghasilkan metode yang lebih akurat untuk memperkirakan usia kematian orang dewasa (WMD=1,96 tahun; 95% CI: -0,88, 4,79) pada seluruh populasi. Metode RDT memberikan akurasi yang lebih baik pada dewasa tua (WMD=1,74 tahun; 95% CI: -2,33, 5,82). Namun, pada kelompok usia dewasa muda dan menengah, akurasi lebih baik pada metode TCA. Perempuan memberikan akurasi yang lebih baik daripada laki-laki pada metode TCA. Kedua metode memberikan korelasi yang cukup kuat terhadap usia kronologis, tetapi metode TCA sedikit lebih reliabel dan berkorelasi lebih kuat dengan usia kronologis. Kesimpulan: Metode RDT lebih akurat dibandingkan dengan metode TCA pada seluruh populasi. Direkomendasikan untuk menggunakan metode TCA untuk dewasa muda dan menengah (15-44 tahun) serta metode RDT untuk dewasa tua (≥45 tahun).

Background: Identification of the living and the dead is essential in routine forensic dental examinations. Several procedures for age-at-death estimation in adults have been introduced, including Tooth Cementum Annulation (TCA) and Root Dentin Translucency (RDT) methods that are frequently used. There are still few studies that compared both methods and their accuracy in estimating adult age at death. Aim: This study aims to test and compare the accuracy between the TCA and RDT methods. Methods: Data searches were carried out through five electronic databases: Pubmed, Scopus, Ebsco, ScienceDirect, and Wiley, following the guidelines of Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA). Results: Out of the total 1178 literature, 28 studies were recruited for qualitative analysis and 23 studies for meta-analysis. RDT produces a more accurate method to estimate age at death for adults (WMD=1.96 years; 95% CI: -0.88, 4.79) in the entire population. The RDT method gave better accuracy in older adults (WMD=1.74 years; 95% CI: -2.33, 5.82). However, in younger adults, the accuracy is better with the TCA method. Furthermore, females give a superior accuracy than males in the TCA age estimation. Both methods give a strong enough correlation to chronological age, but TCA method is slightly more reliable and correlated stronger with chronological age at death. Conclusion: The RDT age estimation is more accurate than the TCA method in the entire population. It is recommended to use the TCA method for younger adults (15-44 years) and the RDT method for the older ones (≥45 years)."
Jakarta: Fakultas Kedokteran Gigi Universitas Indonesia, 2021
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UI - Skripsi Membership  Universitas Indonesia Library
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Philadelphia, PA : Elsevier, 2016
616.994 CLI
Buku Teks  Universitas Indonesia Library
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"The aim of this book is to make the reader familiar with the characteristic signs of disease, including abnormalities of the skin, nerves, eyes, hands, feet, testes, and bone. Early identification of the disease is critical to prevent patient disability and establish appropriate therapy. Emphasis will be given to the current diagnostic tools to identify and quantify the organ damage, including electrophysiology, ultrasonography, magnetic resonance imaging, laboratory tests, and histopathology. Specific topics such as leprosy and pregnancy, leprosy and HIV infection, epidemiology, and leprosy control will also be covered."
Berlin: Springer, 2012
e20410793
eBooks  Universitas Indonesia Library
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"Now, the eighth in the set returns to the topic of brain tumors, dealing with seven distinct types, astrocytoma, medulloblastoma, retinoblastoma, chordoma, craniopharyngioma, oligodendroglioma, and ependymoma. After updating the classification of medulloblastoma the volume provides an overview of ependymoma as well as describing the delineation of prognosis based on the genetic aberrations of the latter patients. The material offers key insights into the molecular pathways involved in tumor biology, such as the role of E-cadherin gene instability, carbonic anhydrase II, urokinase plasminogen activator, and Wnt signaling in meningioma. Contributors explain the genetic and clinical features associated with recurring meningioma, including the role played by erythropoietin receptor, and examine the way in which OTX2 transcription factor functions as an oncogene in medulloblastoma."
Dordrecht: Springer, 2012
e20420776
eBooks  Universitas Indonesia Library
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Tao, Jianguo
"In the last decade, there has been a remarkable explosion of knowledge in hematologic cancer from basic molecular biology and pathology to clinical therapy. This has led to many new advance and insights in the understanding of pathobiology of malignant hematology. New knowledge of disease molecular pathology, cytogenetic, epigenetic and genomic alterations have provided new strategies to attack and eradicate tumor cells at molecular level and significantly impacted our current therapeutics for hematological malignancies. The recent and ongoing rapid expansion of knowledge in this area has become extensive, dynamic and diffuse over the literature and research publications. This has led to the need to capture and compile the new and current information about hematologic cancer with special emphasis on translation from molecular pathobiology to targeted therapeutics. In this book experts from around the world share their thoughts and knowledge about the pathobiology of hematologic cancer, as well as their view on current treatment approaches and future development in these malignant hematologic diseases. "
Dordrecht, Netherlands: Springer, 2012
e20426053
eBooks  Universitas Indonesia Library
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"This is the fifth edition of a very successful textbook on clinical trials methodology, written by recognized leaders who have long and extensive experience in all areas of clinical trials. The three authors of the first four editions have been joined by two others who add great expertise. Most chapters have been revised considerably from the fourth edition. A chapter on regulatory issues has been included and the chapter on data monitoring has been split into two and expanded. Many contemporary clinical trial examples have been added. There is much new material on adverse events, adherence, issues in analysis, electronic data, data sharing, and international trials.
This book is intended for the clinical researcher who is interested in designing a clinical trial and developing a protocol. It is also of value to researchers and practitioners who must critically evaluate the literature of published clinical trials and assess the merits of each trial and the implications for the care and treatment of patients. The authors use numerous examples of published clinical trials to illustrate the fundamentals.
The text is organized sequentially from defining the question to trial closeout. One chapter is devoted to each of the critical areas to aid the clinical trial researcher. These areas include pre-specifying the scientific questions to be tested and appropriate outcome measures, determining the organizational structure, estimating an adequate sample size, specifying the randomization procedure, implementing the intervention and visit schedules for participant evaluation, establishing an interim data and safety monitoring plan, detailing the final analysis plan, and reporting the trial results according to the pre-specified objectives."
Switzerland: Springer International Publishing, 2015
e20509987
eBooks  Universitas Indonesia Library
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New York: William & Wilkins, 1997
R 616.07 STE
Buku Referensi  Universitas Indonesia Library
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"This is a clear, concise and comprehensive reference book for the busy clinician to use in his or her daily patient encounters. It focuses less on etiology, pathophysiology, and epidemiology, and considerably more on practical clinical information. Cancer management information is presented in a reader-friendly format that offers a comprehensive review of each disease along with the most commonly used treatment regimens, including chemotherapy dosing and schedules."
Philadelphia: Lippincott Williams & Wilkins, 2014
616.994 BET
Buku Teks  Universitas Indonesia Library
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Muhammad Maulana
"Latar belakang. Kanker kolorektal merupakan keganasan saluran cerna yang menjadi salah satu penyebab morbiditas dan mortalitas terkait kanker paling banyak di dunia. Perkembangan sel normal menjadi kanker melalui proses mutasi genetik yang membutuhkan waktu bertahun-tahun. Program skrining dapat menurunkan angka kematian namun partisipasinya masih rendah. Saat ini tersedia metode yang bersifat tidak invasif diantaranya dengan dasar pemeriksaan feses yang telah luas digunakan baik sebagai tes tunggal maupun kombinasi. Berbagai metode skrining terus dikembangkan untuk mendapatkan nilai diagnostik yang baik. Dengan mengkombinasikan mRNA CEA feses dan FIT diharapkan dapat menghasilkan metode skrining dengan sensitivitas dan spesifistas yang baik serta terjangkau. Tujuan. Mengevaluasi nilai diagnostik pemeriksaan kombinasi mRNA CEA feses dan FIT dalam mendeteksi lesi neoplastik kolorektal. Metode. Studi potong lintang dengan populasi terjangkau pasien dewasa yang diduga kanker kolorektal di Rumah Sakit Cipto Mangunkusumo pada bulan November 2015 sampai Februari 2016. Analisis uji diagnostik digunakan untuk mendapatkan nilai sensitivitas, spesifisitas, NDP, NDN, RKP dan RKN kombinasi mRNA CEA feses dan FIT dalam mendeteksi lesi neoplastik kolorektal dengan pemeriksaan histopatologi jaringan yang diambil melalui kolonoskopi sebagai baku emas. Lesi neoplastik kolorektal terdiri dari lesi prakanker/adenoma dan kanker.
Hasil. Sebanyak 78 subjek penelitian dengan rerata umur 55,32±12,6 tahun, 73,1% berumur 3 50 tahun dan 53,8% berjenis kelamin pria. Keluhan klinis terbanyak berupa perdarahan nyata saluran cerna 33,3%, nyeri perut 28,2%, dan perubahan pola defekasi 24,4%. Proporsi lesi neoplastik kolorektal sebesar 30,7% terdiri dari prakanker/adenoma 12,8% dan kanker 17,9%. Sensitivitas, spesifisitas, NDP, NDN, RKP dan RKN untuk mendeteksi lesi neoplastik kolorektal berturut turut 75%, 61,11%, 46,07%, 84,66%, 1,93, 0,41; adenoma berturut-turut 50,00%, 50,00%, 12,80%, 87,20%, 1,00, 1,00; dan kanker kolorektal berturut turut 92,86%, 59,37%, 33,26%, 97,44%, 2,29, 0,12. Kesimpulan. Kombinasi mRNA CEA feses dan FIT untuk mendeteksi lesi neoplastik kolorektal di Indonesia memiliki nilai NDN tinggi tetapi sensitivitas, spesifisitas, NDP, RKP dan RKN yang rendah.

Background. Colorectal cancer is one of the gastrointestinal tract malignancy which is one of the most common causes of cancer-related morbidity and mortality in the world. The development of normal cells into cancer through genetic mutations process that take years. Screening programs can reduce mortality rates but low participation. Currently, non-invasive methods are available including the stool based examination which has been widely used as a single test or in combination. Various screening methods continue to be developed to obtain good diagnostic value. By combining faecal CEA and FIT mRNA, it is expected to produce a screening method with good sensitivity and specificity and is affordable. Objective. We aimed to evaluate the diagnostic value of combination faecal mRNA CEA and FIT to detect neoplastic lesions of colorectal Methods. Cross-sectional study with with suspected colorectal cancer at Ciptomangunkusumo Hospital from November 2015 to February 2016. Diagnostic test analysis was used to obtain sensitivity, specificity, PPV, NPV, PLR and NLR of the combination of faecal mRNA CEA and FIT in detecting neoplastic lesions of colorectal by histopathological examination of tissues taken through colonoscopy as the gold standard. Colorectal neoplastic lesions consist of precancerous/adenoma and cancerous lesions.
Results. A total of 78 subjects with a mean age of 55.32±12.6 years, 73.1% aged older than fifty and 53.8% were male. The most clinical complaints were obvious gastrointestinal bleeding 33.3%, abdominal pain 28.2%, and changes in bowel habits 24.4%. The proportion of colorectal neoplastic lesions was 33.3% consisting of 15.4% precancer/adenoma and 17.9% cancer. Sensitivity, specificity, PPV, NPV, PLR and NLR for detecting colorectal neoplastic lesions was 75%, 61.11%, 46.07%, 84.66%, 1.93, 0.41 respectively; adenoma 50.00%, 50.00%, 12.80%, 87.20%, 1.00, 1.00 repectively; colorectal cancer 92.86%; 59.37%; 33.26%; 97.44%; 2.29; 0.12 respectively. Conclusion. The combination of faecal CEA mRNA and FIT in detecting colorectal neoplastic lesions has high NPV but low sensitivity, specificity, PPV, PLR and NLR.
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Jakarta: Fakultas Kedokteran Universitas Indonesia, 2022
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UI - Tesis Membership  Universitas Indonesia Library
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