5 research outputs found
Additional file 1: of Selection bias and subject refusal in a cluster-randomized controlled trial
Sample screening form. The standardized form that study coordinators completed for each patient screened for eligibility. (PDF 213 kb
Additional file 2: of Selection bias and subject refusal in a cluster-randomized controlled trial
ICARE study protocol. A document describing the full study protocol, including screening and recruitment procedures. (PDF 6937 kb
DataSheet_1_Small cell lung cancer with dermatomyositis: a case report.docx
Dermatomyositis represents an autoimmune disorder characterized by notable skin and muscular manifestations. The annual incidence of dermatomyositis stands at approximately (5~10)/1 million individuals. Notably, patients with malignant tumors exhibit an elevated risk of developing dermatomyositis compared to the general population. However, in cases where dermatomyositis co-occurs with malignancy, the efficacy of hormone therapy alone tends to be suboptimal. Moreover, reports addressing the correlation between tumor treatment and the management of dermatomyositis are scarce. A 60-year-old male patient presented with dermatomyositis, initially manifesting through symptoms such as rash, muscle weakness, and dysphagia. Despite undergoing standard hormone therapy, there was no discernible improvement in the dermatomyositis symptoms. Considering the patient’s concomitant troublesome cough, further investigations were conducted, including CT, PET-CT, and pathological biopsy. These assessments confirmed the diagnosis of limited-stage small cell lung cancer (T1cN3M0 IIIB). Notably, in this patient, dermatomyositis was suspected to be a paraneoplastic syndrome associated with small cell lung cancer. Standard chemotherapy and radiotherapy were employed to treat the small cell lung cancer, resulting in partial remission after two treatment cycles. As the malignancy regressed, a notable improvement in dermatomyositis symptoms was observed, subsequently leading to a gradual reduction in the prescribed hormone dosage. In conclusion, we present a comprehensive case study of dermatomyositis as a paraneoplastic syndrome throughout the treatment process. The response to tumor therapy coincided with the amelioration of dermatomyositis symptoms. Therefore, diligent malignancy screening is imperative for patients diagnosed with dermatomyositis.</p
Polysarcosine as PEG Alternative for Enhanced Camptothecin-Induced Cancer Immunogenic Cell Death
Nanomedicine-enhanced
immunogenic cell death (ICD) has attracted
considerable attention for its great potential in cancer treatment.
Even though polyethylene glycol (PEG) is widely recognized as the
gold standard for surface modification of nanomedicines, some shortcomings
associated with this PEGylation, such as hindered cell endocytosis
and accelerated blood clearance phenomenon, have been revealed in
recent years. Notably, polysarcosine (PSar) as a highly biocompatible
polymer can be finely synthesized by mild ring-opening polymerization
(ROP) of sarcosine N-carboxyanhydrides (Sar-NCAs)
and exhibit great potential as an alternative to PEG. In this article,
PSar-b-polycamptothecin block copolymers are synthesized
by sequential ROP of camptothecin-based NCAs (CPT-NCAs) and Sar-NCAs.
Then, the detailed and systematic comparison between PEGylation and
PSarylation against the 4T1 tumor model indicates that PSar decoration
can facilitate the cell endocytosis, greatly enhancing the ICD effects
and antitumor efficacy. Therefore, it is believed that this well-developed
PSarylation technique will achieve effective and precise cancer treatment
in the near future
DataSheet_1_Sintilimab plus autologous NK cells as second-line treatment for advanced non-small-cell lung cancer previous treated with platinum-containing chemotherapy.docx
This pilot study (NCT03958097; https://www.clinicaltrials.gov/ct2/show/NCT03958097) was aimed to evaluate the efficacy and safety of PD-1 antibody combined autologous NK cells in the treatment of patients with stage IIIB/IIIC or IV non-small-cell lung cancer (NSCLC) who failed the first-line platinum-based chemotherapy. All patients received both sintilimab 200mg and 3×109 NK cells every 3 weeks. 20 patients were enrolled, median follow up time was 22.6 months. The median PFS was 11.6 months, ORR was 45%. Median OS was 17.7 months, 6-month OS rate and 12-month OS rate was 95.0% and 80.0%. Unexpected adverse events were not observed. 2 patients reported grade 3 adverse events (hypertriglyceridemia, neutropenia and increased creatine kinase). The autologous NK cells did not add extra adverse events to the ICI treatment. Autologous NK plus sintilimab showed promising antitumor activity and an acceptable safety profile in advanced driven-mutation negative NSCLC who failed on the first line treatment.</p