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  1. Dzarr AA, Kamal M, Baba AA
    Eur J Oncol Nurs, 2009 Sep;13(4):250-4.
    PMID: 19386547 DOI: 10.1016/j.ejon.2009.03.006
    This study assessed the agreement between infrared tympanic membrane (TM), axillary, corrected axillary (+0.5 degrees C), oral, and corrected oral (+0.3 degrees C) to rectal thermometry as reference standard in neutropenic adults. The sensitivity and specificity of the mentioned thermometries in detecting rectal fever (> or =38 degrees C) were also analysed.
  2. Jennise Tan Teng Teng, Mohd Yuhazri Yaakob, Haeryip Sihombing, Abu Abdullah, Suriati Akmal
    MyJurnal
    Honeycomb with good mechanical properties and low density are the top priorities in
    material selection. Therefore, the facesheet thickness is a factor that contributes to it
    as it made up most of the weight in the structure. Appropriate thickness can optimize
    the mechanical performance. However, the sandwich composite may associate to high
    density if the facesheet is of high thickness yet deteriorate the mechanical properties
    as an overall. As the facesheet is attached to the sandwich structure via matrix, the
    peeling properties for various facesheet thickness is investigated. The facesheet
    thickness in terms of one to five layers are glued to the rubber wood core. The
    structures are tested for its peeling strength under vertical 90° test according to the
    ASTM standard. The optimal number of facesheet with good peeling strength is
    discussed
  3. Ankathil R, Azlan H, Dzarr AA, Baba AA
    Pharmacogenomics, 2018 04;19(5):475-393.
    PMID: 29569526 DOI: 10.2217/pgs-2017-0193
    Despite the excellent efficacy and improved clinical responses obtained with imatinib mesylate (IM), development of resistance in a significant proportion of chronic myeloid leukemia (CML) patients on IM therapy have emerged as a challenging problem in clinical practice. Resistance to imatinib can be due to heterogeneous array of factors involving BCR/ABL-dependent and BCR/ABL-independent pathways. Although BCR/ABL mutation is the major contributory factor for IM resistance, reduced bio-availability of IM in leukemic cells is also an important pharmacokinetic factor that contributes to development of resistance to IM in CML patients. The contribution of polymorphisms of the pharmacogenes in relation to IM disposition and treatment outcomes have been studied by various research groups in numerous population cohorts. However, the conclusions arising from these studies have been highly inconsistent. This review encompasses an updated insight into the impact of pharmacogenetic variability on treatment response of IM in CML patients.
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