2025 Volume 27 Issue 11 Published: 28 November 2025
  

  • Select all
    |
  • Guidelines for pharmaceutical care of granulocyte-stimulating factors in cancer patients (2024 edition)
    National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital of Chinese Academy of Medical Sciences and Peking Union Medical College, Oncology Specialty Pharmacist Branch of the Chinese Pharmacists Association
    2025, 27(11): 641-653. https://doi.org/10.3760/cma.j.cn114015-20250624-00327
    Abstract ( ) PDF ( )
    Neutropenia is the most common hematological toxicity in chemotherapy for cancer patients. Granulocyte colony-stimulating factors (G-CSF) are currently the most commonly used symptomatic therapeutic drugs in clinical practice, playing a key role in ensuring adequate doses and on schedule in chemotherapy. As of December 2024, more than 80 specifications of G-CSF have been approved for market in China, which provides diverse options in clinical practice while also poses higher demands on standardized management of pharmaceutical services. Therefore, the Oncology Specialty Pharmacists Branch of the Chinese Pharmacists Association, in collaboration with the National Cancer Center and multidisciplinary experts nationwide, jointly formulated this guideline by integrating clinical evidence, relevant regulations on pharmaceutical affairs management, and pharmaceutical service practices. The development process involves systematic literature search, Delphi method, expert interviews, and discussions. The key pharmacological service points of G-CSF in cancer patients were systematically elaborated in this guideline, covering aspects such as indication management, dosage and administration, medication for special populations, combined medication strategies, economic evaluation, and adverse reaction monitoring, resulting in 22 recommendations. This guideline aims to provide a systematic and scientific reference for the rational use of G-CSF and related pharmaceutical services for cancer patients.
  • Analysis of the reasons for medication errors in deslanoside injection use
    Li Siyan, Zhang Qingxia, Medication Safety Panel in China Core Group of International Network for the Rational Use of Drugs
    2025, 27(11): 654-659. https://doi.org/10.3760/cma.j.cn114015-20250117-00037
    Abstract ( ) PDF ( )
    Objective To explore the causes of medication errors (ME) associated with deslanoside injection and put forward targeted preventive recommendations. Methods ME reports related to deslanoside injection in the National Monitoring Network for Clinical Safe Medication (Monitoring Network) as of August 31, 2024 were collected, and sever ME cases of deslanoside injection were also collected though searching medical literature databases at home and abroad, China Judgements Online, and PKULAW database at the same period. The level of severity, occurrence link, error content, occurrence place, trigger personnel and patient outcomes of the MEs were retrospectively analyzed. Results The Monitoring Network received a total of 41 ME reports of deslanoside injection from September 2012 to August 2024, and the number of reports showed an upward trend year by year. These MEs were classified as grade A in 1 case (2.4%), grade B in 18 cases (43.9%), grade C in 17 cases (41.5%), grade D in 4 cases (9.8%), and grade F in 1 case (2.4%). There were 63.4% (26/41) of MEs occurring in the prescription/doctor′s order prescribing and delivery links, mainly caused by physicians, and the common error contents included solvent errors, medication under contraindications, and having drug-drug interactions. In addition, 26.8% (11/41) of MEs occurred in the drug dispensing and distribution link, and 9.8% (4/41) occurred in the administration and monitoring links. A total of 4 severe MEs of deslanoside injection were collected from the Monitoring Network, medical literature and judicial cases, all of which occurred in the prescription/doctor′s order prescribing and delivery links. Among the 4 severe MEs, 2 ME cases of grade I occurred due to incorrect usage and dosage, resulting in patient death; 1 ME case of grade F was caused by interaction with traditional Chinese medicine, resulting in digitalis poisoning, and another case of grade F was that deslanoside injection was administered to a patient with digitalis poisoning (medication under contraindications). Conclusions MEs of deslanoside injection often occurs in the prescription/doctor′s order prescribing and delivery links, mainly because of insufficient knowledge of doctors to the drug instructions. It is suggested to strengthen learning and training of medical staff centered around drug instructions, and improve the system interception and process management, so as to improve the medication safety.
  • Clinical safety of sodium-glucose cotransporter 2 inhibitors: a study based on adverse drug reaction monitoring data in Beijing from 2019 to 2024
    Xie Yue, Song Zhihui, Liu Junhan, Zhao Huiying, Zhang Guojuan, Wang Jiawei
    2025, 27(11): 660-666. https://doi.org/10.3760/cma.j.cn114015-20250108-00019
    Abstract ( ) PDF ( )
    Objective To analyze the characteristics of adverse reactions of sodium-glucose cotransporter 2 inhibitors (SGLT2i), and provide a basis for the rational clinical application. Methods The adverse drug reaction (ADR) cases of SGLT2i reported by Beijing from January 1, 2019 to June 30, 2024 were collected through searching the National Adverse Drug Reaction Monitoring System of China. The Medical Dictionary for Regulatory Activities (MedDRA) terminology set was used to standardize the description of ADR, and the involving system organ class (SOC) and preferred term (PT) was extracted. Data of ADR were analyzed descriptively and statistically. Results A total of 409 SGLT2i-related adverse reaction reports involving 409 patients were included. Among these patients, there were 232 females and 177 males; the median age was 62(52, 70) years, and 231 cases (56.48%) were under the age of 65 years; 5 types of SGLT2i (dapagliflozin, empagliflozin, canagliflozin, ertugliflozin, and henagliflozin proline) were involved, and reports of dapagliflozin was the most (279 cases, 68.22%). The primary indication for medication was diabetes (404 cases, 98.78%). The majority of ADRs did not reach the severe level (395 cases, 96.58%). The 14 cases (3.42%) of severe ADR were primarily about diabetic ketoacidosis (11 cases, 11/14), of which 7 cases presented with normal blood glucose levels and 5 cases occurred after medical stress events. The outcomes of patients were improvement in 241 cases (58.92%) and recovery in 127 cases (31.05%). In total, 476 ADR occurrences were recorded among the 409 patients, involving 82 PTs, 24 of which were not listed in the drug labels. The top 2 SOCs were the infections and infestations [26.26% (125/476)] and renal and urinary disorders [13.87% (66/476)]; the top 3 PTs were urinary tract infection [23.32% (111/476)], urinary ketone detection [6.51% (31/476)], and vulvovaginal pruritus [5.88% (28/476)]; the top 3 newly identified possible ADRs (PTs) were dizziness [2.31% (11/476)], palpitations [1.89% (9/476)], and decreased appetite [1.05% (5/476)]. Conclusions Based on the ADR monitoring data in Beijing in the past 5 and a half years, SGLT2i-associated adverse reactions primarily involved the infections and infestations, and renal and urinary disorders. ADRs identified in the study such as dizziness and palpitations are not documented in the drug labels,  euglycaemic ketoacidosis accounts for a high proportion of severe reactions, and most of them occur after acute stress events. 
  • Literature case analysis of nephrogenic systemic fibrosis induced by gadolinium-based contrast agents in patients with nephropathy
    Liu Di, Yu Hong, Cao Jianping, Meng Xiaobin
    2025, 27(11): 667-673. https://doi.org/10.3760/cma.j.cn114015-20250205-00053
    Abstract ( ) PDF ( ) Supplementary files
    Objective To explore the occurrence and clinical characteristics of nephrogenic systemic fibrosis (NSF) induced by gadolinium-based contrast agents (GBCA). Methods CNKI, Wanfang, VIP and PubMed databases were searched (as of October 28, 2024) and case reports on GBCA-related NSF were collected; the following information was extracted, including the publication year of the literature, country, patient gender, age, basic kidney diseases and renal replacement therapy, variety of GBCA used, exposure frequency, time of occurrence or diagnosis of NSF, clinical manifestations, pathological examination, main intervention measures and outcomes. The data were analyzed by descriptive statistics. Results A total of 45 case reports were collected, involving 97 patients. The literature were reported mainly from the United States and published mainly in 2006 and 2007. Number of the relevant literature decreased significantly after 2008, but there were still new cases reports in China in the following years (for example, in 2023). Among the 97 patients, 53 (54.6%) were male and 44 (45.4%) were female; the age ranged from 9 to 83 years with a median age of 53 years. One patient was with severe malnutrition, while the other 96 had severe basic kidney diseases, including chronic kidney disease in 85 (88.5%) patients and acute kidney injury in 11 (11.5%) patients. Variety of GBCA exposed was described in 76 patients, including gadodiamide in 67 (88.2%) patients. Exposure frequency of GBCA before NSF occurrence was described in 88 patients, 48 (54.5%) of which were exposed only once and 23 (26.1%) were exposed twice. Time from the first GBCA exposure to the occurrence of NSF was described in 92 patients, with the shortest time of 2 days and the longest time of more than 10 years; 70.7% (65/92) occurred within 3 months after GBCA exposure. All patients had typical skin symptoms of NSF, which were confirmed by pathological examination. Among them, 43 (44.3%) had joint disorders, 9 patients had eye involvement, a few patients had cardiac fibrosis, respiratory failure, metabolic acidosis, rhabdomyolysis, muscle necrosis, etc. Follow-up information was described in 82 patients with a range of 4 months to 11 years. Among them, 21 patients (25.6%) died, mainly due to the basic kidney diseases and complications; 11 (13.4%) were severely disabled; 7 (8.5%) were mildly disabled or slowly deteriorated; 43 (52.4%) had stable disease or slightly improved condition. Conclusion NSF caused by GBCA mainly occurs in patients with severe basic renal diseases, mostly caused by gadodiamide. Severe skin damage is often accompanied by joint involvement or even disability, and the overall prognosis is poor.
  • Analysis of 408 cases of tigecycline-related adverse reactions
    Liu Xiao, Lin Jingyu, Zhao Simiao, Zheng Bo, Zhou Ying
    2025, 27(11): 674-680. https://doi.org/10.3760/cma.j.cn114015-20250305-00117
    Abstract ( ) PDF ( )
    Objective To analyze the clinical characteristics of tigecycline-related adverse reactions and provide the basis for the safe and rational use of the drug. Methods Adverse reaction reports with suspected drug as tigecycline from Beijing Adverse Drug Reaction Monitoring Center from January 1st, 2019 to June 30th, 2024 were collected. The adverse reaction reports were standardized using the preferred term (PT) and system organ class (SOC) in the Chinese updated edition (2015 version) of the World Health Organization Adverse Reaction Terminology. The patients′ general condition, tigecycline use, and adverse reaction occurrence (including latency, severity, treatment, outcome, and correlation evaluation) were descri- ptively and statistically analyzed. Results A total of 408 tigecycline-related adverse reaction reports were entered, including 153 females (37.5%) and 255 males (62.5%). The age was (68±21) years, ranging from 2 to 99. The main reasons for tigecycline use were infections of lung, blood flow, skin and skin soft tissue, etc. The pathogens were mainly Klebsiella pneumoniae, Acinetobacter baumanii, Escherichia coli, etc. The usage and dosage of tigecycline in most patients were in line with the instructions. Four hundred and eight adverse event reports involved 11 SOCs and 580 PTs. The top 3 SOCs were gastrointestinal diseases (195 case times, 33.62%), vascular, bleeding and coagulation diseases (183 case times, 31.55%), and hepatobiliary diseases (142 case times, 24.48%). The main clinical manifestations were nausea, vomiting, diarrhea, etc. The main laboratory abnormalities were decreased plasma fibrinogen, decreased platelet count, increased alanine aminotransferase, increased aspartate aminotransferase, and increased bilirubin. There were 27 case times of adverse reactions that were not recorded in the instructions, mainly including leukopenia, abdominal distension, fever, dysbacteriosis, etc. The latency of adverse reactions ranged from 5 min to 65 days, with a median time of 5 days. The grade of adverse reactions was general in 379 patients (92.89%) and severe in 29 patients (7.11%). The top 3 SOCs involved in 53 case times of severe adverse reactions were hepatobiliary diseases (30 case times, 56.60%), vascular, bleeding and coagulation diseases (8 case times, 15.09%), and urinary tract diseases (4 case times, 7.55%), the main clinical manifestations were elevated liver enzymes, coagulation disorders, pancreatitis, etc. After the occurrence of adverse reactions, all patients stopped tigecycline, and received symptomatic treatments such as liver protection, intravenous infusion of human fibrinogen, intravenous infusion of platelets, and antidiarrheal therapy. Among 408 patients, 66 (16.18%) were cured, 297 (72.79%) were improved, 20 (4.90%) were not improved, and 25 cases′ outcome (6.13%) were unknown. The shortest time for recovery or improvement was 0.5 hour, the longest was 44 days, with a median time of 5 days. The correlation between tigecycline and adverse reactions was probable in 132 patients (32.35%), and possible in 276 patients (67.65%). Conclusions Tigecycline-related adverse reactions involve multiple organ systems, mainly including gastrointestinal diseases, vascular, bleeding and coagu- lation diseases, and hepatobiliary diseases, etc. which can lead to severe adverse reactions such as acute pancreatitis and coagulation disorders. After drug withdrawal and symptomatic treatments, most patients had a good prognosis.
  • Clinical characteristics of warfarin-related nephropathy: a retrospective case series study
    Chen Nana, Liu Wenqi, Li Junsheng, Guo Dequn, Sun Guiling, Li Zhengrong
    2025, 27(11): 681-685. https://doi.org/10.3760/cma.j.cn114015-20250331-00173
    Abstract ( ) PDF ( )
    Objective To analyze the clinical characteristics of warfarin-related nephropathy (WRN). Methods Medical records of patients with WRN admitted to Linyi People′s Hospital Affiliated to Shandong Second Medical University from January 1, 2020 to December 31, 2024 were collected. The patients′ basic information (gender, age), warfarin medication details (indications, dosage, frequency, etc.), comorbidities, concomitant medication usage, international normalized ratio (INR) and serum creatinine (Scr) test results before and after the occurrence of WRN, as well as the clinical manifestations, interventions, and outcomes of WRN were extracted. The causal relationship between warfarin and renal dysfunction was evaluated according to the Adverse Drug Reaction Reporting and Monitoring Manual. The clinical data of patients were descriptively and statistically analyzed. Results A total of 11 patients were entered in the analysis, including 7 males and 4 females; the age ranged from 49 to 85 years, with a median age of 70 years, and 9 cases were older than 60 years. The causality evaluation showed that 3 patients were definite and 8 patients were probable. All the 11 patients had at least one comorbidity, including 6 cases of heart failure, 6 cases of hypoproteinemia, 4 cases of chronic kidney disease, 3 cases of hypertension, 3 cases of pulmonary infection, and 1 case of diabetes. Seven patients were treated with warfarin combined with broad-spectrum antibiotics, 6 combined with diuretics, and 3 combined with renin angiotensin system blockers. The time from the highest INR to the highest Scr level was 0-6 days, with a median time of 2 days, and it was ≤2 days in 9 patients. Six patients had bleeding manifestations such as microscopic hematuria, melena, epistaxis, hematochezia, and skin ecchymosis. Among the 11 patients, 10 stopped warfarin immediately and 1 reduced dosage. All patients received different doses of vitamin K1  according to the INR level. Among the 6 patients of bleeding, 4 received symptomatic treatments such as omeprazole, tranexamic acid, somatostatin, thrombin powder and octreotide, and 2 patients received hemodialysis due to high Scr level. One patient with severe anemia received blood transfusion. After 1-5 days of treatments (with a median time of 2 days), the INR in all patients decreased to <3.00, of which 5 patients continued to take warfarin, 1 changed warfarin to rivaro- xaban, and 5 did not continue anticoagulation therapy. After 2 to 14 days of treatments, Scr in 8 patients recovered to the reference value range, and Scr in 3 patients was still at a high level, of which 1 patient died of unexplained cardiac arrest. Conclusions WRN is a common adverse reaction of warfarin, with or without bleeding. After the occurrence of WRN, the drug should be stopped as soon as possible and symptomatic treatment should be given. The prognosis is generally good, but it may also lead to chronic kidney disease.
  • Risk signal mining and analysis of adverse events in agalsidase beta therapy for Fabry disease
    Li Zongyun, Jiao Jiaxun, Gao Lingna, Zhu Xiaoli
    2025, 27(11): 686-693. https://doi.org/10.3760/cma.j.cn114015-20250417-00206
    Abstract ( ) PDF ( )
    Objective To mine risk signals of adverse events (AE) in agalsidase beta therapy for Fabry disease and provide reference for the safe use in clinical practice. Methods The AE reports with agalsidase beta as the primary suspect drug in the US Food and Drug Administration Adverse Event Reporting System (FAERS) database from the first quarter of 2004 to the third quarter of 2024 were collected and the clinical information of patients involved was analyzed descriptively. AEs were standardized and categorized using the preferred term (PT) and system organ class (SOC) in Medical Dictionary for Regulatory Activities version 26.0. Signal mining was performed using the reporting odds ratio (ROR) method and Bayesian confidence propagation neural network (BCPNN) method. A PT was defined as the risk signal if the number of reports was ≥3, the lower limit of the 95% confidence interval (CI) of ROR was >1, and the information component minus two times standard deviation (IC025) was >0. Descriptive statistical analysis were then conducted on the risk signals. The relative risk of target adverse events in gender subgroups was evaluated using the ROR method. Results A total of 24 163 AE reports with agalsidase beta as the primary suspect drug were collected, involving 7 763 patients and 2 382 PTs. Severe adverse events accounted for 34.9% (2 712/7 763). A total of 121 risk signals (namely PTs) across 15 SOCs were obtained. The top 5 PTs ranked by number of reports were pyrexia (483 cases), chills (449 cases), infusion related reaction (282 cases), chest pain (221 cases), and cerebrovascular accident (218 cases). The top 5 PTs ranked by signal intensity were cornea verticillata (ROR=56.44, IC025=4.59), drug specific antibody present (ROR=54.13, IC025=5.46), cerebral calcification (ROR=24.82, IC025=3.16), myocardial necrosis marker increased (ROR=24.14, IC025=3.83), and infusion site rash (ROR=20.41, IC025=3.46). Among the top 30 PTs ranked by number of reports and signal intensity, there were 4 and 13 PTs not documented in the drug label, respectively. The former included atrial fibrillation, cellulitis, neuralgia, and pallor, while the latter included cornea verticillate, cerebral calci- fication, auricular swelling, vein discoloration, aortic dilatation, bundle branch block, myocardial fibrosis, cardiac infection, vein rupture, sudden hearing loss, meningitis viral, deafness transitory, and corneal opacity. Subgroup analysis by sex showed that males had higher risks in developing chills, tremor, drug specific antibody detection, renal failure, and renal impairment, while females had higher risks in weight increase and dizziness. Conclusions The main risk signals of adverse events of agalsidase beta include pyrexia, chills, and infusion related reactions, which are consistent with those documented in package inserts. In addition, potential new risk signals such as atrial fibrillation, cellulitis, neuralgia, cornea verticillate, auricular swelling, and sudden hearing loss were also detected. The relative risks of some target adverse events vary between genders, and it is recommended to strengthen targeted drug monitoring and individuali- zed management in clinical practice.
  • Nephrotic syndrome with acute kidney injury induced by cetuximab
    Sun Lei, Ning Jie, Wang Fang, Rao Jing, Jiang Jiemei
    2025, 27(11): 694-696. https://doi.org/10.3760/cma.j.cn114015-20240731-00661
    Abstract ( ) PDF ( )
    A 59-year-old male patient with sigmoid colon cancer and liver metastasis received the treatments of cetuximab combined with FOLFIRI regimen (irinotecan, calcium folinate, and fluorouracil). His serum creatinine (Scr) was 82 μmol/L, and estimated glomerular filtration rate (eGFR) was 96 ml/(min·1.73 m2) before the treatment. On the 11th day after finishing the 4th cycle of treatments, the patient deve- loped nausea and vomiting.Laboratory tests showed Scr 221 μmol/L, eGFR 29 ml/(min·1.73 m2), serum albumin 29.0 g/L, urinary protein (+++), and 24 hour urine protein quantified 8.88 g. He was diagnosed as having nephrotic syndrome complicated with acute kidney injury, which was considered to be related to cetuximab. The drug was stopped and symptomatic treatments such as anti-inflammatory, anticoagulation and kidney protection were given. After 14 days, laboratory tests showed no proteinuria, Scr 156 μmol/L, and eGFR 44 ml/(min·1.73 m2). Prednisone acetate tablet 50 mg were orally administered once daily. Fifty-nine days later, his Scr was 142 μmol/L, and eGFR was 49 ml/(min·1.73 m2). Chemotherapy was suspended and cetuximab was discontinued permanently.
  • Hypotension and syncope with acute kidney injury caused by the combination of simnotrelvir/ritonavir and benidipine
    Xu Zhilian
    2025, 27(11): 696-698. https://doi.org/10.3760/cma.j.cn114015-20241219-00214
    Abstract ( ) PDF ( )
    A 69-year-old male patient with hypertension was treated with long-term oral admini- stration of benidipine (8 mg, once daily) and losartan (100 mg, once daily). Due to the novel coronavirus infection, he took simnotrelvir/ritonavir (1.5 g of simnotrelvir, 0.1 g of ritonavir) by himself. After 10 hours, he experienced syncope and unconsciousness. His blood pressure was 70/40 mmHg, heart rate was 40 times/min, and consciousness recovered about 15 minutes later. Laboratory tests showed B-type natriuretic peptide 233 ng/L and blood creatinine 188 μmol/L. Electrocardiogram showed atrial fibrillation. Color Doppler ultrasound of the heart showed enlargement of both atria. Head CT showed suspicious low-density shadows in the brainstem and left frontal lobe. Immediate symptomatic treatments including fluid replacement, blood pressure increase with norepinephrine and dopamine, and anticoagulation with enoxaparin sodium were given. Antihypertensive drugs were stopped. After 1 day of symptomatic treatments, the patient′s blood pressure was 130-150/60-80 mmHg, norepinephrine and dopamine were discontinued. Three days after antihypertensive medication withdrawal, the patient′s blood pressure was 168/80 mmHg, and antihy- pertensive treatments were resumed (levoamlodipine 2.5 mg twice daily orally, sacubitril and valsartan 100 mg once daily orally). Eleven days later, the patient′s blood pressure was 114-135/74-78 mmHg, and blood creatinine was 96 μmol/L. It was considered that the hypotension and syncope were caused by the combination of simnotrelvir/ritonavir and benidipine, and the acute kidney injury was a prerenal injury caused by hypotension.
  • Amphotericin B liposome-induced acute cardiac dilatation and heart failure in a pediatric patient
    Dai Enpeng, Chen Yuan, Yang Shibin, Wang Pan, Tian Ya
    2025, 27(11): 699-702. https://doi.org/10.3760/cma.j.cn114015-20241114-00150
    Abstract ( ) PDF ( )
    An 8-year-old male patient with chronic granulomatous disease received amphotericin B liposome (unknown dose) in addition to anti-infection treatments with meropenem, compound sulfamethoxazole, and voriconazole due to recurrence of secondary pulmonary infection. After 3 days, the patient developed tachycardia, edema, and worsening dyspnea. Echocardiography revealed severe right heart enlarge- ment and pulmonary hypertension. Cardiotonic, diuretic, and pulmonary antihypertensive therapies were given. After over half a month, his pulmonary infection was improved, pulmonary arterial pressure decrea- sed, but the right heart enlargement persisted. Suspending treatment about half a month later, amphotericin B liposome was reinitiated at a gradually increased dose from 2 mg once daily, in combination with piperacillin sodium and tazobactam sodium and compound sulfamethoxazole due to aggravated cyanosis and cough. After the administration of amphotericin B liposome (50 mg once daily) on day 5, the patient experienced wheezing and facial edema. Laboratory tests showed B-type natriuretic peptide (BNP) 4 679 ng/L; echocardiography demonstrated right heart enlargement and pulmonary hypertension. Suspecting that the cardiac dilatation and heart failure were associated with amphotericin B liposome, the drug was discon- tinued. The anti-infection regimen was switched to biapenem, linezolid and voriconazole, along with conti- nued cardiotonic and diuretic managements. The patient′s symptoms were improved after 10 days, the treatment regimen was changed to compound sulfamethoxazole and voriconazole. However, after 3 days, the patient′s abdominal distension and dyspnea worsened. Endotracheal intubation and mechanical ventilation were initiated along with cardiotonic and diuretic therapy; anti-infection therapy with cefoperazone sodium and sulbactam sodium combined with voriconazole was given based on bronchoalveolar lavage fluid and sputum culture results. One month later, the patient′s condition was improved, showing no right ventricular dilation and reduced pulmonary arterial pressure on echocardiography and BNP 800 ng/L.
  • Intestinal perforation following anlotinib treatment in a non-small cell lung cancer patient
    Wang Chunyan, Cao Shoubo, Wu Bing, Heng Rui, Ling Wei, Weng Guixiang
    2025, 27(11): 702-704. https://doi.org/10.3760/cma.j.cn114015-20250106-00011
    Abstract ( ) PDF ( )
    A 75-year-old male patient with non-small cell lung cancer in the lower lobe of the left lung underwent left lobectomy, followed by 4 cycles of adjuvant chemotherapy with paclitaxel and platinum, 4 cycles of chemotherapy with docetaxel and cisplatin, and immunotherapy with sintilimab, 13 cycles of immunotherapy with sintilimab monotherapy, and 5 cycles of endostatin and sintilimab, spanning a total of 5 years. Due to disease progression, he received the monotherapy with anlotinib, 42 days later, the patient developed intestinal perforation, and laparoscopic ileal perforation repair surgery was performed. During the operation, a perforation with a diameter of about 1 cm was observed in the ileum, indicating the outflow of digestive fluid and a large amount of purulent fluid accumulation in the pelvic cavity; no signs of gastrointestinal tumor metastasis were observed. After surgery, the patient developed abdominal infection and peritonitis, and was given symptomatic and supportive treatments such as anti-infection for 7 days. However, the patient developed severe complications such as lung infection, heart failure, sepsis, and respiratory failure, and died.
Office
Journal
Download
More...
Link
More...