Miao Qiuli, Liu Yang, Wang Haiying, Li Tingyu
Objective To explore the clinical characteristics of pembrolizumab-induced immune- mediated encephalitis (IME) and provide reference for clinical medication safety. Methods Domestic and international databases were searched (up to December 31, 2024), and case reports on pembrolizumab- related IME were collected. Data on patient basic information, pembrolizumab use, time to IME onset, and the clinical manifestations, auxiliary examinations, treatments and outcomes of IME were extracted for descriptive statistical analysis. Results A total of 21 articles involving 21 patients were included. There were 15 males and 6 females, aged 64 (56, 71) years with a range of 47-80 years. Primary diseases included lung cancer in 9 patients, melanoma in 6 patients, and myxoid chondrosarcoma, nasal angiosarcoma, thyroid cancer, bladder cancer, renal cell carcinoma, and uterine cancer in 1 patient each. Twenty patients received pembrolizumab monotherapy, and 1 received the drug combined with paclitaxel (albumin-bound). The time from pembrolizumab initiation to IME onset was recorded in 20 cases, which was 147 (90, 267) days with a range from 21 to 360 days. Main clinical manifestations of IME included cognitive impairment (12 cases), motor/sensory deficits (9 cases), psychiatric/behavioral abnormalities (7 cases), consciousness disturbance (7 cases), epileptic seizures (6 cases), and autonomic dysfunction (2 cases). Regarding the auxiliary examinations, abnormal electroencephalogram accounted for 10/11; abnormal cerebrospinal fluid analysis accounted for 14/16, mainly characterized by elevated protein and increased lymphocyte/white blood cell counts; abnormal cranial MRI accounted for 50.0% (10/20), and the abnormal signals were frequently observed in the temporal lobe (hippocampal) or white matter/subcortical regions. After IME onset, 18 patients received glucocorticoid therapy, 5 of whom also received human immunoglobulin and 2 received additional plasma exchange; the other 3 patients were treated solely with human immunoglobulin, an antipsychotic agent (aripiprazole), and an antiepileptic regimen (sequential therapy with levetiracetam and valproate), respectively. Pembrolizumab was discontinued in 19 patients. Of them, the condition was improved in 16 patients, remained stable in 2 patients, and was not improved in 1 patient (died later). The other 2 patients did not stop pembrolizumab and both showed clinical improvement in IME, however, one of them subsequently died due to acute massive cerebral infarction complicated by hemorrhage. Conclusion Clinical manifestations and auxiliary examinations of pembrolizumab-induced IME lack specificity. Most patients have a favorable prognosis after discontinuation of pembrolizumab and treatments with glucocorticoids and/or human immunoglobulin. Making decision on whether to continue pembrolizumab or not requires an individualized evaluation of the patient′s specific condition.
