Prognosis Clinical Trial
Official title:
Thyroid Biological Toxicity and Tumor Response in Patients Treated With NIVOLUMAB 2nd Line in Non-small Cell Bronchopulmonary Cancer
This is an observational, retrospective and monocentric study, conducted at the university Hospital of Brest The primary objective is to assess the association between the occurrence of thyroid dysfunction in patients treated with Nivolumab® for a non-small cell lung cancer and prognosis and therapeutic response The second objective is to assess prognosis and therapeutic response according to severity and subtype of thyroid dysfunction
Cohort characteristics
The patients' characteristics were collected from medicals records: age, gender, smoking
status (absent, current or weaned), WHO performance index, neoplastic characteristics (tumor
histology, history of brain metastasis, prior radiotherapy treatment, prior therapy lines
(defined by the number of chemotherapy or immunotherapy regimens used before Nivolumab®
treatment) We also recorded data about expression of tumor PD-L1, LDH levels and the
lymphocyte to neutrophil ratio (dNLR) summarized in the LIPI score (Lung immune prognostic
index), which distinguishes three categories: good prognosis (normal LDH, dNLR <3),
intermediate prognosis (abnormal LDH or dNLR> 3), poor prognosis (abnormal LDH and dNLR> 3),
Treatment schedule and morphological monitoring
Nivolumab® (3mg/kg mg) was administered as an IV infusion for 30 minutes every 2 weeks until
disease progression, unacceptable toxicity, or death. Tumor assessment was performed every 2
months until disease progression. Tumor assessment was based on the results of the
computerized tomodensitometry (CT) + injection of a radioiodine contrast agent and/or
18F-fluorodeoxyglucose (FDG) positron emission tomography (PET/CT) (18FDG-PET/CT), according
to the RECIST 1.1 or iRECIST 1.1 ((immune) Response Evaluation Criteria in Solid Tumors)
criterion. In case of a dissociated response (response of a lesion associated with a
progression of another lesion) or in case of suspicion of pseudo-progression (increase in
size or appearance of new lesions linked to the influx of immune cells within the tumor), a
new morphological evaluation after two additional cycles was taken into account.
Thyroid function screening and classification of thyroid dysfunction
Thyroid function screening was performed before (<3 months) and during treatment with
Nivolumab® (TSH, free T4 (fT4), free T3 (fT3) ± Anti-thyroid peroxidase antibodies (TPOAb)
and/or TSH receptor antibodies (TRAbs) were measured by electrochemiluminescence (Reference
laboratory values were: TSH, 0.27-4.20 mIU/L; fT4, 11.6-22.0 pmol/L; fT3, 4.0-6.8 pmol/L;
TPOAb, <34 kIU/L; and TRAb, <1.75 U/L
For classification of thyroid dysfunction, the CTCAE classification was not taken into
account because it is not adapted to thyroid dysfunction that is often asymptomatic. Only
abnormalities of the thyroid function tests were considered as follow:
1. Patients with abnormalities of TSH level were classified in the group "Thyroid
Dysfunction +" and those with normal TSH level were classified in the group "Thyroid
Dysfunction -". In case of normal TSH with isolated abnormality of peripherical hormone
fT4 and/or fT3, the patient was classified in the "Thyroid Dysfunction -" group;
2. Depending on the level of peripheral thyroid hormones (i.e. fT3 and fT4): subclinical
thyroid dysfunction was defined by an abnormal TSH without abnormality of the peripheral
hormones and overt thyroid dysfunction was defined by an abnormal TSH associated with at
least one abnormality of the peripheral hormones T3 or T4L;
3. Depending on the TSH level: moderate thyroid dysfunction was defined by a TSH level
between 0.1 mIU/L and 0.27 mIU/L or between 4.2 mIU/L and 10 mIU/L, and severe thyroid
dysfunction was defined in case of TSH ≤ 0.1 mUI/L or ≥ 10 mUI/L, respectively for
hyperthyroidism and hypothyroidism;
4. Depending on the type of thyroid dysfunction, we classified each patient in three
categories isolated hypothyroidism, isolated thyrotoxicosis and thyroiditis
(thyrotoxicosis then hypothyroidism).
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