Evaluation of clinicopathological factors in PD-1 response: derivation and validation of a prediction scale for response to PD-1 monotherapy

Nosrati, Adi; Tsai, Katy K.; Goldinger, Simone M.; Tumeh, Paul C.; Grimes, Barbara; Loo, Kimberly; Algazi, Alain P.; Nguyen-Kim, Thi Dan Linh; Levesque, Mitchell P.; Dummer, Reinhard; Hamid, Omid; Daud, Adil

doi:10.1038/bjc.2017.70

Cited by 115 publications

(105 citation statements)

References 36 publications

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“…In the seventh edition, an elevated LDH level was used to categorize a patient as M1c, regardless of anatomic site(s) of metastatic disease, given its significance as an independent, adverse predictor of survival among patients with stage IV disease. LDH remains a clinically significant factor associated with response, progression‐free survival, MSS, and overall survival in the contemporary treatment era of targeted and immune therapies . In the eighth edition, an elevated LDH level no longer independently defines M1c disease.…”

Section: Major Changesmentioning

confidence: 99%

“…LDH remains a clinically significant factor associated with response, progression-free survival, MSS, and overall survival in the contemporary treatment era of targeted and immune therapies. [75][76][77] In the eighth edition, an elevated LDH level no longer independently defines M1c disease. Instead, to better codify the impact of anatomic site and LDH level, descriptors were added to the M1 subcategory designation to indicate LDH status (designated as "[0]" for not elevated and " [1]" for elevated) for each M1 subcategory ( Table 4).…”

Section: Serum Ldh Levelmentioning

confidence: 99%

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Melanoma staging: Evidence‐based changes in the American Joint Committee on Cancer eighth edition cancer staging manual

Gershenwald

Scolyer

Hess

et al. 2017

CA A Cancer J Clinicians

1,806

1,704

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To update the melanoma staging system of the American Joint Committee on Cancer (AJCC) a large database was assembled comprising >46,000 patients from 10 centers worldwide with stages I, II, and III melanoma diagnosed since 1998. Based on analyses of this new database, the existing seventh edition AJCC stage IV database, and contemporary clinical trial data, the AJCC Melanoma Expert Panel introduced several important changes to the Tumor, Nodes, Metastasis (TNM) classification and stage grouping criteria. Key changes in the eighth edition AJCC Cancer Staging Manual include: 1) tumor thickness measurements to be recorded to the nearest 0.1 mm, not 0.01 mm; 2) definitions of T1a and T1b are revised (T1a, <0.8 mm without ulceration; T1b, 0.8–1.0 mm with or without ulceration or <0.8 mm with ulceration), with mitotic rate no longer a T category criterion; 3) pathological (but not clinical) stage IA is revised to include T1b N0 M0 (formerly pathologic stage IB); 4) the N category descriptors “microscopic” and “macroscopic” for regional node metastasis are redefined as “clinically occult” and “clinically apparent”; 5) prognostic stage III groupings are based on N category criteria and T category criteria (ie, primary tumor thickness and ulceration) and increased from 3 to 4 subgroups (stages IIIA–IIID); 6) definitions of N subcategories are revised, with the presence of microsatellites, satellites, or in-transit metastases now categorized as N1c, N2c, or N3c based on the number of tumor-involved regional lymph nodes, if any; 7) descriptors are added to each M1 subcategory designation for lactate dehydrogenase (LDH) level (LDH elevation no longer upstages to M1c); and 8) a new M1d designation is added for central nervous system metastases. This evidence-based revision of the AJCC melanoma staging system will guide patient treatment, provide better prognostic estimates, and refine stratification of patients entering clinical trials.

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Section: Major Changesmentioning

confidence: 99%

Section: Serum Ldh Levelmentioning

confidence: 99%

Melanoma staging: Evidence‐based changes in the American Joint Committee on Cancer eighth edition cancer staging manual

Gershenwald

Scolyer

Hess

et al. 2017

CA A Cancer J Clinicians

1,806

1,704

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“…A recently revealed clinical trend shows some association with liver metastases and reduced responses to αPD‐1 across cancer types in melanoma, urothelial cancer, TNBC and NSCLC . However, there are some conflicting results with some studies reporting no associations with liver metastases .…”

Section: Discussionmentioning

confidence: 99%

“…Evidence has recently emerged for the tumor location influencing the response of human tumors to immunotherapies, particularly to αPD‐1 and αPD‐1/αCTLA4 . In particular, retrospective analysis has revealed reduced responses to checkpoint blockade in tumors in certain metastatic sites compared with primary tumors in melanoma, non‐small‐cell lung cancer (NSCLC), urothelial cancer and triple‐negative breast cancer (TNBC) . Due to the complexity of tumors at different anatomical sites, including tumor genetic heterogeneity, the tissue‐specific impact on therapy responses in human tumors is yet to be elucidated.…”

Section: Introductionmentioning

confidence: 99%

Tissue‐specific tumor microenvironments influence responses to immunotherapies

et al. 2019

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Objectives Investigation of variable response rates to cancer immunotherapies has exposed the immunosuppressive tumor microenvironment (TME) as a limiting factor of therapeutic efficacy. A determinant of TME composition is the tumor location, and clinical data have revealed associations between certain metastatic sites and reduced responses. Preclinical models to study tissue‐specific TMEs have eliminated genetic heterogeneity, but have investigated models with limited clinical relevance. Methods We investigated the TMEs of tumors at clinically relevant sites of metastasis (liver and lungs) and their impact on αPD‐1/αCTLA4 and trimAb (αDR5, α4‐1BB, αCD40) therapy responses in the 67NR mouse breast cancer and Renca mouse kidney cancer models. Results Tumors grown in the lungs were resistant to both therapies whereas the same tumor lines growing in the mammary fat pad (MFP), liver or subcutaneously could be completely eradicated, despite greater tumor burden. Assessment of tumor cells and drug delivery in 67NR lung or MFP tumors revealed no differences and prompted investigation into the immune TME. Lung tumors had a more immunosuppressive TME with increased myeloid‐derived suppressor cell infiltration, decreased T cell infiltration and activation, and decreased NK cell activation. Depletion of various immune cell subsets indicated an equivalent role for NK cells and CD8+ T cells in lung tumour control. Thus, targeting T cells with αPD‐1/αCTLA4 or trimAb was not sufficient to elicit a robust antitumor response in lung tumors. Conclusion Taken together, these data demonstrate that tissue‐specific TMEs influence immunotherapy responses and highlight the importance in defining tissue‐specific response patterns in patients.

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“…[37] В общей сложности в данный анализ было включено 315 пациентов с метастатической меланомой, получавших пембролизумаб (2 или 10 мг/кг каждые 2 недели или каждые 3 недели) или ниволумаб (3 мг/кг каждые 2 недели) в четырех онкологических центрах в период с 2011 по 2013 г. Переменные, имеющие стати-стически значимую связь с ответом на лечение при одно-мерном анализе, вводили в модель пошагового логисти-ческого регрессионного анализа и получали баллы на основе относительного риска для расчета клинической шкалы прогноза (табл. 9, 10).…”

Section: признакunclassified

Pembrolizumab in the Treatment of Metastatic Melanoma

Самойленко¹,

Демидов²

2017

Med. sov.

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Evaluation of clinicopathological factors in PD-1 response: derivation and validation of a prediction scale for response to PD-1 monotherapy

Cited by 115 publications

References 36 publications

Melanoma staging: Evidence‐based changes in the American Joint Committee on Cancer eighth edition cancer staging manual

Melanoma staging: Evidence‐based changes in the American Joint Committee on Cancer eighth edition cancer staging manual

Tissue‐specific tumor microenvironments influence responses to immunotherapies

Pembrolizumab in the Treatment of Metastatic Melanoma

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