2024 Volume 26 Issue 9 Published: 28 September 2024
  

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  • Yin Yue, Zhang Yanhua
    Abstract ( ) PDF ( )
    Drugs or their metabolites may accumulate in the body due to the decline of renal excretion function in cancer patients with renal insufficiency. Therefore, adjusting the treatment scheme and drug dose according to the patient′s renal function is an important part of anticancer treatment for these patients. The Japanese Society of Nephrology, Japan Society of Clinical Oncology, Japanese Society of Medical Oncology, and Japanese Society of Nephrology and Pharmacotherapy have jointly formulated Clinical Practice Guidelines for Management of Kidney Injury During Anticancer Drug Therapy 2022, and specifically discusses the dose adjustment of anticancer drug treatment for patients with renal injury in the second chapter.
    This article focuses on the interpretation of the application and dose adjustment of antifolate agents, BCRABL1 tyrosine kinase inhibitors, epithelial growth factor receptor tyrosine kinase inhibitors, antibody molecularly targeted agents and tumor adjuvant therapy drugs such as bone‑modifying agents in patients with renal injury in this chapter. 
  • Lin Zhiqiang
    Abstract ( ) PDF ( )
    Unsafe medication and medication errors are the main causes of avoidable harm in the health system. In order to reduce drug?related harm, it is necessary to pay special attention to medication safety in high?risk situations, medication safety during polypharmacy, and medication safety during the transitions of medical care. The main factors leading to high?risk situations include drugs (high?alert drugs), human (drug provider and patient), and environment (drug management, treatment environment and human resources, etc.). Strengthening management for polypharmacy can promote the rational use of drugs and minimize drug?related harm. Reducing medication errors and/or adverse drug events in transitions of care requires collaboration from multiple parties, including interdisciplinary care teams such as physicians, pharmacists, and nurses, as well as active participation from patients and their families. Compared with developed countries, there is still a significant gap in the 3 areas in China, and physicians, pharmacists, and nurses need to take active actions and make joint efforts to ensure the medication safety of patients.
  • Zheng Yuan, Yan Chen, Li Bin, Li Zhengxiang, Yuan Hengjie
    Abstract ( ) PDF ( )
    Objective To mine the adverse events (AE) of nervous system caused by epidermal growth factor receptor (EGFR) inhibitors, and provide reference for the safe use of EGFR inhibitors in clinics. Methods AE of nervous system caused by gefitinib, erlotinib, afatinib and osimertinib were searched from FDA Adverse Drug Event Reporting System (FAERS) database using OpenVigil data platform from 2004, 2004, 2013, and 2015 to the 2nd quarter of 2023, respectively. The AE was standardized using the preferred term (PT) in the Medical Dictionary for Regulatory Activities 23.0 version. Data such as patient general condition and AE of nervous system was extracted from AE reports and was analyzed descriptively. Reporting odds ratio (ROR) and proportional reporting ratio (PRR) methods were used for detection of AE signal of nervous system. AE that simultaneously met the following conditions was considered as a risk signal: the number of report cases ≥3, lower limit of the 95% confidence interval of ROR≥1, PRR≥2, and χ2≥4. Results A total of 422 nervous system AE cases related to gifitinib were collected, involving 297 patients and 42 preferred terms (PT); 10 risk signals were detected, including dementia, brain oedema, demyelina- tion, leukoencephalopathy, hemiplegia, vocal cord paralysis, neurological symptom, cerebral atrophy, intracranial pressure increase and neuropathy, with 64 AE cases involved. One thousand seven hundred and fifty?five nervous system AE cases related to erlotinib were collected, involving 1?477 patients and 69 PT; 7 risk signals were detected, including ageusia, hyperaesthesia, facial pain, demyelination, motion sickness, vocal cord paralysis, peripheral paralysis, with 142 AE cases involved. Two hundred and forty?seven nervous system AE cases related to afatinib were collected, involving 212 patients and 32 PT; 7 risk signals were detected, including ageusia, cerebral infarction, brain oedema, epilepsy, central nervous system lesion, leukoencephalopathy, cerebral disorder, with 49 AE cases involved. Six hundred and fifty?two nervous system AE cases related to osimertinib were collected, involving 582 patients and 46 PT; 3 risk signals were detected, including cerebral infarction, vocal cord paralysis, facial paralysis, with 54 AE cases involved. Ageusia was an AE already included in the label of afatinib, while other AE were not included. Conclusion Most of the EGFR inhibitor?related AE signals found in the FAERS database are not included in the labels, and should be monitored during the clinical use.
  • Li Yuan, Zhang Wenwen, Zhang Yuchen
    Abstract ( ) PDF ( )
    Objective To mine risk signals of adverse events (AE) related to methylphenidate in children, and provide insights for the safe clinical use of the drug. Methods AE reports of children with methylphenidate as primary suspect drug were collected from the US FDA Adverse Event Reporting System (FAERS) database during the 1st quarter of 2004 to the 1st quarter of 2023. The AEs were standardized and classified using the preferred term (PT) and system organ class (SOC) of the Medical Dictionary for Regulatory Activities 26.0, and the reporting odds ratio (ROR) method and Bayesian confidence propagation nerve (BCPNN) method were used respectively to mine the AE risk signals of the drug. An AE with reports
    ≥3, the lower limit of the 95%CI of ROR>1,and information component (IC)-2SD>0 was defined as a risk signal. Descriptive analysis on the risk signals was performed. Results A total of 13?777 reports were collected. Two hundred risk signals were obtained using ROR and BCPNN method, involving 18 SOCs. Top 10 PTs in the number of reports were decreased appetite, aggression, headache, insomnia, agitation, psychomotor hyperactivity, anxiety, irritability, tics, and suicidal ideation, of which suicidal ideation was not recorded in the label; the SOCs involved were psychiatric disorders, metabolism and nutrition disorders, nervous system disorders. Top 10 PTs by signal strength were coronary artery dissection, Huntington′s disease, zoophobia, nail picking, polydipsia, lip?biting disorder, Alice in Wonderland syndrome, depression, onychophagia, and dermatillomania, all adverse reactions except depression were not recorded in the label; the SOCs involved were cardiac disorders, various congenital familial genetic disorders, and psychiatric disorders. Conclusions The main AEs related to methylphenidate in children are decreased appetite, aggression, headache, insomnia, and other adverse reactions recorded in the label. However, methylpheni- date may also lead to adverse reactions such as suicidal ideation, coronary artery dissection, Huntington′s disease, nail picking, and other adverse reactions not recorded in the label. Clinicians and pharmacists should be vigilant during the use of methylphenidate.
  • Zhang Cijia, Song Yanqing, Zhang Hongmei
    Abstract ( ) PDF ( )
    To explore the clinical characteristics of pembrolizumab?related type 1 diabetes mellitus (T1DM). Methods The relevant databases (up to August 31, 2023) were searched and the basic information of patients, application of pembrolizumab, combination medication, the occurrence of T1DM, laboratory test results, clinical manifestation, treatment and prognosis were analyzed descriptively and statistically. Results A total of 48 patients (from 46 articles) were included in the analysis, including 27 males and 21 females, aged from 12 to 85 years with a median age of 64 years. The primary diseases were mainly lung cancer and melanoma. Thirty-eight patients had records of time from medication to diagnosis of T1DM, which was 21?660 days (a median time of 84 days). Of the 48 patients, 41 developed diabetes ketoacidosis (DKA), and 10 developed fulminant T1DM. The main clinical manifestations were polyuria, polydipsia, and thirst, and some patients had dyspnea or disturbance of consciousness. Forty?five patients had blood glucose testing records, with blood glucose levels ranging from 9.1 to 69.7?mmol/L and a median blood glucose level of 31.8?mmol/L; 43 cases had records of glycated hemoglobin testing, of which 36 cases had glycated hemoglobin ≥6.5%; 35 cases had serum C?peptide detection records, and 30 cases had serum C?peptide below the lower limit of the reference value. After being diagnosed with T1DM, 35 patients stopped pembrolizumab, 2 cases did not discontinue, and 11 cases had no relevant records; 46 patients received insulin therapy and 2 cases had no relevant records. Among the 48 patients, 2 patients′ blood glucose returned to normal, 22 patients′ blood glucose was well controlled, 1 patient′s condition deteriorated, 1 patient′s tumor progressed, 4 patients died, and 18 patients′ prognosis was not reported. Among 35 patients who stopped using pembrolizumab, 11 patients restarted immunotherapy. Conclusions The clinical manifestations of pembrolizumab?related T1DM are similar to those of common T1DM, but the incidence of DKA is higher. Half of the patients′ blood glucose can be well controlled after insulin treatment.
  • Zhao Manman, He Runcheng, Yang Ying, Zuo Zeping, Cao Xinyao, Wang Chao, Wen Nie, Wang Sanlong, Geng Xingchao, Wang Zhibin, Zhou Xiaobing
    Abstract ( ) PDF ( )
    To explore the effects of maternal exposure to Morinda officinalis oligosaccharides (MOO) during lactation on the Sprague?Dawley (SD) maternal rats and their offspring′s growth and development. Methods Seventy?two female rats with a surviving litter size of ≥ 6 were divided into the excipients control group, MOO low?dose group (50?mg/kg), MOO medium?dose group (160?mg/kg), and MOO high?dose group (500?mg/kg) using a snake-shaped grouping based on body weight, with 18 rats per group. The rats were gavage fed once daily until 20 days of delivery. The response of maternal rats after MOO exposure during lactation, as well as the appearance, response, gross anatomical abnormalities of their F1 and F2 offspring were observed. The body weight and food intake of maternal rats during lactation and those of their offspring before and after weaning were measured. The behavior (central nervous system function) of the F1 and F2 offspring was evaluated using functional observation battery (FOB). The learning and memory function of the F1 offspring was evaluated using Y?maze test. The male and female F1 offspring in the same dose group were mated when they were raised to 10?12 weeks in order to observe the reproductive function of F1 female rats. Results Compared with the excipients control group, no abnormality was found in the clinical observation of maternal rats in the 3 MOO exposure groups during lactation, and there was no significant differences in their body weight and daily food intake during lactation (all P>0.05). No significant effects were found on the appearance, clinical symptoms, gross anatomy, body weight, and food intake of the F1 and F2 offspring after maternal rats receiving MOO exposure during lactation. In the FOB of the F1 and F2 offspring and the Y?maze test of F1 offspring, few differences in MOO exposure groups were observed and lack of significant dose?response relationship. After pregnancy, there were no statistically significant differences in the number of corpus luteum, implantation number, birth index, delivery index, survival index, and weaning index in F1 female offspring of maternal rats exposed to MOO at different doses during lactation compared with those of the excipients control group (all P>0.05). Conclusions There were no obvious toxic reactions in maternal rats after exposure to different doses of MOO during lactation, nor in the growth and development, nervous system, learning and memory, and reproductive function of their offspring.
  • Xing Xiaomin, Li Xiangpeng, Quan Xianghua, Wang Xinyi, Wang Wenxiao, Li Jing
    Abstract ( ) PDF ( )
    Objective To establish a prescription pre⁃audit system based on the structureprocess⁃outcome (SPO) model in the the Affiliated Hospital of Qingdao University and explore its application effect. Methods Based on the structural dimension of SPO model, the organizational structure, pharmaceutical team, management system of pharmaceutical prescription audit, and audit environment of the prescription pre⁃audit system were established. Based on the process dimension of SPO model, the preaudit process, medication knowledge base, and audit rule base were established, quality monitoring and control were implemented, and relevant personnel training were conducted. Based on the outcome dimension of SPO model, the review rate, manual review rate, clinician acceptance rate of prescription review, reasonable rate of outpatient and emergency prescription comments, and intervention rate of inpatient medical order were verified after the prescription pre⁃audit system application. Results The prescription preaudit system was first launched in the main hospital area of the Affiliated Hospital of Qingdao University in March 2021, and achieved full coverage in all five hospital areas by May 2023. The review rates of outpatient and emergency prescriptions and inpatient medical orders had been increasing year by year from 2021 to 2023, and all reached more than 99% of the expected rates in 2023. Compared with 2021, the proportions of outpatient and emergency prescriptions and inpatient medical orders submitted to manual review decreased in 2023
    [1.2% (112 206/9 509 430) vs. 2.9% (16 214/549 672), 2.9% (206 258/7 152 620) vs. 3.9% (147 679/3 814 929), the proportions of prescriptions that failed to be reviewed in time decreased [0.7% (62 382/9 509 430) vs. 1.4% (7 429/549 672), 0.3% (22 816/7 152 620) vs. 2.2% (83 303/3 814 929)], and the acceptance rates of outpatient and emergency prescription review and inpatient medical orders review by clinicians increased [76.1% (2 421/3 180) vs. 57.0% (339/595), 94.3% (1 000/1 060) vs. 70.7% (797/1 128)],
    with statistically significant differences (all P<0.001). But there were still some prescriptions and orders that needed manual review but were not reviewed in time and finally missed review. Compared with 2021, the reasonable rates of outpatient and emergency prescription comments increased in 2023 [96.7% (924 558/956 252) vs. 92.2% (983 827/1 067 357), 98.7% (518 307/525 227) vs. 98.0% (181 296/185 069)], and the intervention rate of inpatient medical orders decreased [0.7% (196 522/26 751 992) vs. 0.9% (195 660/22 631 289)], with statistically significant differences (all P<0.001). Conclusions Applying the SPO model can improve the organization and management of the prescription pre⁃audit system, and ensure the smooth launch and safe operation of the system. After verification, the operating speed of the prescription pre⁃audit system and prescription review speed of pharmacists could basically meet the clinical needs, the indicators of rational drug use in the hospitals were improved, and the professional and technical ability of pharmacists were enhanced.
  • Zhang Yunxia, Qin Qianqian, Zhao Ruiling, Wang Xiaoling
    Abstract ( ) PDF ( ) Supplementary files
    Objective To investigate the reasons for contraindication of chemical drugs and biological products that were marked as contraindication for children in drug labels in China. Methods The drugs labeled as contraindication for children in drug labels of chemicals and biological products covered by the China Pharmacopoeia 2020 and the 2023 China′s Basic Medical Insurance, Work?related Injury Insurance and Childbirth Insurance (western medicine) were searched. The reasons of contraindication for children were collected through searching the drug labels, Clinical Medication Instructions of the China Pharmacopoeia 2020, the website of the National Medical Products Administration, and drug labels from the Unite States, and analyzed descriptively. Results There were 222 drugs were labeled as contraindication for children in the drug labels, involving 20 categories and mainly antibiotics and digestive system drugs. Among 222 drugs, 137(61.7%) had the reasons for contraindication in pediatric patients, and the main reasons were adverse drug reactions (65.7%, 90/137) and lack of effectiveness and safety information yet in children (30.7%, 42/137), followed by the unsafe auxiliary materials (1.5%, 2/137), unsuitable pres- cription design or ingredients for children (1.5%, 2/137) and unsuitable dosage form for children (0.7%, 1/137). The above reasons were collected from domestic drug instructions (100 drugs), U.S. drug labels (17 drugs), NMPA website instructions revision announcements and popular science knowledge (15 drugs), and Clinical Medication Instructions of the China Pharmacopoeia 2020 (5 drugs). Conclusions It is relatively common in China to label drugs that are contraindicated for children without specifying the reasons for contraindication or with non?standard explanations in the instructions. Therefore, it is necessary to further standardize the contraindication information for children and apply continuous updates and improvement in order to provide timely and up?to?date drug use information for clinical practice.
  • Chen Minting, Liu Yan, Ma Jie, Zheng Ke
    Abstract ( ) PDF ( )
    A 53‑year‑old female patient with bone metastasis of breast cancer received targeted drugs (abemaciclib 150 mg orally twice daily, exemestane 25 mg orally once daily), zoledronic acid (4 mg IV infusion once per month), traditional Chinese medicine, and non‑steroidal anti‑inflammatory drugs. After 2 months, her serum creatinine (Scr) increased from 84 μmol/L before treatment to 156 μmol/L. Due to renal tissue puncture biopsy, the patient missed taking abemaciclib for 1 day. The laboratory tests next day showed that her Scr decreased from 151 μmol/L to 123 μmol/L. Comparing the estimated glomerular filtration rate calculated using serum cystatin C with that calculated using Scr, combined with the pathological examination results of renal biopsy tissue, the patient′s renal injury caused by other drugs could be ruled out, and the possibility of pseudo‑elevation of Scr caused by abemaciclib was considered.
  • Abstract ( ) PDF ( )
    A 36-year-old healthy male served as an allogeneic hematopoietic stem cell donor was given recombinant human granulocyte colony-stimulating factor injection (rhG-CSF) 300 μg by subcutaneous injection once daily for 5 consecutive days. On day 4 of stem cell mobilization, peripheral stem cell collection was performed and rhG-CSF 250 μg was given in addition. The donor experienced dry cough, dyspnea, and difficulty breathing on the next day. Chest CT scan showed diffuse patchy and nodular shadows in both lungs, and relevant tests excluded bacterial/viral infection of the lungs and heart failure. It was considered to be acute lung injury caused by rhG-CSF. After giving glucocorticoids and symptomatic treatments, the symptoms gradually subsided, and the peripheral blood stem cell collection was successful. In the continuing treatment of glucocorticoids, the symptoms of the donor were further improved, and chest CT scan showed marked improvement. At a 3 years of follow-up, the donor‘work and life were normal, and no lung discomfort symptoms recurred.
  • Wang Huimin
    Abstract ( ) PDF ( )
    A 40-year-old female patient took Kangfuyan capsules 1.2 g (3 capsules) thrice daily orally by herself for cervical erosion. After 10 days of treatment, the patient developed anorexia and nausea; after taking the drug intermittently for about 30 days, the symptoms were not improved. Laboratory tests showed alanine aminotransferase (ALT) 793?U/L,aspartate aminotransferase (AST) 699 U/L, total bilirubin (TBil) 27.4 μmol/L, and alkaline phosphatase (ALP) 130 U/L. Drug-induced liver injury was diagnosed, which was considered to be related to Kangfuyan capsules. The drug was stopped, and the liver-protective treatments were given. Sixteen days later, the above symptoms in the patient were improved, laboratory tests showed ALT 79 U/L, AST 55 U/L, and ALP 79 U/L; 30 days later, laboratory tests showed ALT 44 U/L, AST 40 U/L, ALP 51 U/L, and TBil 21.5 μmol/L.
  • Qu Jingrong, Zhang Lei
    Abstract ( ) PDF ( )
    A 15-year-old female child with juvenile idiopathic arthritis for 10 years received methotrexate combined with adalimumab (80?mg by subcutaneous injection once every 2 weeks) 2 years ago. After 1.5 years of treatments, red papules appeared on the skin of the perineum and thigh, accompanied by itching.The rash gradually spread to multiple parts of the body, including the head,neck, and limbs, with plaques and scales, and the rash on both calve ruptures and oozes, accompanied by itching and pain. It was considered to be severe atopic dermatitis caused by adalimumab based on skin pathological results, elevated serum immunoglobulin E, and clinical signs. The results of the patient′s wound secretion culture indicated a mixed infection of resistant bacteria such as Staphylococcus aureus, Pseudomonas aeruginosa, and Enterococcus faecalis. After discontinuing adalimumab and receiving systemic treatments with anti?allergic and sensitive antibiotics, as well as local treatment with glucocorticoids for 14 days, the rash and infection were improved. At the six?month of follow-up, the patient′s skin lesions were basically healed.
  • Xie Yajun, Zhao Bei, Li Shixing, Li Xiaoye, Shi Ning
    Abstract ( ) PDF ( )
    A 61-year-old male patient with coronary heart disease was treated with dual antiplatelet therapy, lipid-lowering therapy (atorvastatin) and other symptomatic drugs after coronary interventions. Because the patient was at ultra-high-risk of cardiovascular events, had multiple in-stent restenosis, and had uncontrolled blood lipids, subcutaneous injection of evolocumab 140?mg was added once every 2 weeks. The platelet count (PLT) of the patient was within the reference range before evolocumab application. After 2 injections of evolocumab, he developed bloody sputum, blood blisters on the lips and scattered bleeding points around the body, with PLT 19×109/L. The dual antiplatelet therapy and evolocumab were suspended, but the bleeding was aggravated. According to the results of bone marrow puncture and biopsy, the patient was diagnosed with idiopathic thrombocytopenic purpura. Glucocorticoid, human immunoglobulin, recombinant human thrombopoietin and platelet transfusion were given but not effective. Subsequently, herombopag was added and PLT gradually increased. After 25 days, the PLT was 109×109/L.