“Metastatic Cancer of Unknown Primary” or “Primary Metastatic Cancer”?

Cancer of unknown primary (CUP) is an umbrella term used to classify a heterogeneous group of metastatic cancers based on the absence of an identifiable primary tumor. Clinically, CUPs are characterized by a set of distinct features comprising early metastatic dissemination in an atypical pattern, an aggressive clinical course, poor response to empiric chemotherapy and, consequently, a short life expectancy. Two opposing strategies to change the dismal prognosis for the better are pursued. On the one hand, following the traditional tissue-gnostic approach, more and more sophisticated tissue-of-origin (TOO) classifier assays are employed to push identification of the putative primary to its limits with the clear intent of allowing tumor-site specific treatment. However, robust evidence supporting its routine clinical use is still lacking, notably with two recent randomized clinical trials failing to show a patient benefit of TOO-prediction based site-specific treatment over empiric chemotherapy in CUP. On the other hand, with regards to a tissue-agnostic strategy, precision medicine approaches targeting actionable genomic alterations have already transformed the treatment for many known tumor types. Yet, an unmet need remains for well-designed clinical trials to scrutinize its potential role in CUP beyond anecdotal case reports. In the absence of practice changing results, we believe that the emphasis on finding the presumed unknown primary tumor at all costs, implicit in the term CUP, has biased recent research in the field. Focusing on the distinct clinical features shared by all CUPs, we advocate adopting the term primary metastatic cancer (PMC) to denominate a distinct cancer entity instead. In our view, PMC should be considered the archetype of metastatic disease and as such, despite accounting for a mere 2–3% of malignancies, unraveling the mechanisms at play goes beyond improving the prognosis of patients with PMC and promises to greatly enhance our understanding of the metastatic process and carcinogenesis across all cancer types.

[1]  Metastatic , 2020, Definitions.

[2]  B. Chauffert,et al.  A phase III trial of empiric chemotherapy with cisplatin and gemcitabine or systemic treatment tailored by molecular gene expression analysis in patients with carcinomas of an unknown primary (CUP) site (GEFCAPI 04) , 2019, Annals of Oncology.

[3]  N. Pavlidis,et al.  Familial cancer of unknown primary , 2019, International Journal of Clinical Oncology.

[4]  A. Jemal,et al.  Annual Report to the Nation on the Status of Cancer, Featuring Cancer in Men and Women Age 20–49 Years , 2019, Journal of the National Cancer Institute.

[5]  A. Krämer,et al.  Does Cancer of Unknown Primary (CUP) Truly Exist as a Distinct Cancer Entity? , 2019, Front. Oncol..

[6]  Yan Yang,et al.  Complete response to crizotinib in a metastatic adenocarcinoma of unknown primary harboring MET amplification and NTRK1 co-occurring mutation , 2019, OncoTargets and therapy.

[7]  J. Blay,et al.  Molecular screening program to select molecular-based recommended therapies for metastatic cancer patients: analysis from the ProfiLER trial. , 2019, Annals of oncology : official journal of the European Society for Medical Oncology.

[8]  F Levi,et al.  European cancer mortality predictions for the year 2019 with focus on breast cancer. , 2019, Annals of oncology : official journal of the European Society for Medical Oncology.

[9]  P. Keegan,et al.  FDA Approval Summary: Pembrolizumab for the Treatment of Microsatellite Instability-High Solid Tumors , 2019, Clinical Cancer Research.

[10]  P. Zhao,et al.  Carcinoma of Unknown Primary with EML4-ALK Fusion Response to ALK Inhibitors. , 2019, The oncologist.

[11]  H. Mukai,et al.  Randomized Phase II Trial Comparing Site-Specific Treatment Based on Gene Expression Profiling With Carboplatin and Paclitaxel for Patients With Cancer of Unknown Primary Site. , 2019, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[12]  C. Brennan,et al.  Tumor mutational load predicts survival after immunotherapy across multiple cancer types , 2019, Nature Genetics.

[13]  C. Dive,et al.  Molecular characterisation and liquid biomarkers in Carcinoma of Unknown Primary (CUP): taking the ‘U’ out of ‘CUP’ , 2018, British Journal of Cancer.

[14]  N. Hattori,et al.  ROS1-rearranged putative lung adenocarcinoma presenting as carcinoma of unknown primary site: a case report , 2018, Oncotarget.

[15]  A. Jemal,et al.  Global cancer statistics 2018: GLOBOCAN estimates of incidence and mortality worldwide for 36 cancers in 185 countries , 2018, CA: a cancer journal for clinicians.

[16]  S. Luoh,et al.  When Tissue Is No Longer the Issue: Tissue-Agnostic Cancer Therapy Comes of Age , 2018, Annals of Internal Medicine.

[17]  W. Erber,et al.  Genetic characterisation of molecular targets in carcinoma of unknown primary , 2018, Journal of Translational Medicine.

[18]  Elaine R. Mardis,et al.  The emerging clinical relevance of genomics in cancer medicine , 2018, Nature Reviews Clinical Oncology.

[19]  J. Swensen,et al.  Comprehensive analysis of cancers of unknown primary for the biomarkers of response to immune checkpoint blockade therapy. , 2018, European journal of cancer.

[20]  M. Berger,et al.  Patient HLA class I genotype influences cancer response to checkpoint blockade immunotherapy , 2018, Science.

[21]  N. Hattori,et al.  Putative lung adenocarcinoma with epidermal growth factor receptor mutation presenting as carcinoma of unknown primary site , 2018, Medicine.

[22]  N. Schultz,et al.  Clinical and molecular characterization of patients with cancer of unknown primary in the modern era , 2017, Annals of oncology : official journal of the European Society for Medical Oncology.

[23]  Joon-Oh Park,et al.  Correlating programmed death ligand 1 (PD-L1) expression, mismatch repair deficiency, and outcomes across tumor types: implications for immunotherapy , 2017, Oncotarget.

[24]  P. Stephens,et al.  Tumor Mutational Burden as an Independent Predictor of Response to Immunotherapy in Diverse Cancers , 2017, Molecular Cancer Therapeutics.

[25]  J. Rodríguez HLA-mediated tumor escape mechanisms that may impair immunotherapy clinical outcomes via T-cell activation , 2017, Oncology letters.

[26]  S. Lippman,et al.  Utility of Genomic Analysis In Circulating Tumor DNA from Patients with Carcinoma of Unknown Primary. , 2017, Cancer research.

[27]  Manel Esteller,et al.  Precision medicine based on epigenomics: the paradigm of carcinoma of unknown primary , 2017, Nature Reviews Clinical Oncology.

[28]  Marie-Cécile Le Deley,et al.  High-Throughput Genomics and Clinical Outcome in Hard-to-Treat Advanced Cancers: Results of the MOSCATO 01 Trial. , 2017, Cancer discovery.

[29]  Donavan T. Cheng,et al.  Mutational Landscape of Metastatic Cancer Revealed from Prospective Clinical Sequencing of 10,000 Patients , 2017, Nature Medicine.

[30]  O. Røe,et al.  The undifferentiated carcinoma that became a melanoma: Re-biopsy of a cancer of an unknown primary site: a case report , 2017, Journal of Medical Case Reports.

[31]  C. von Kalle,et al.  Integration of genomics and histology revises diagnosis and enables effective therapy of refractory cancer of unknown primary with PDL1 amplification , 2016, Cold Spring Harbor molecular case studies.

[32]  M. Hirano,et al.  [A Case of Axillary Nodal Metastasis of Adenocarcinoma of an Unknown Primary Site Effectively Treated with Anti-HER2plus AC plus Paclitaxel Therapy]. , 2016, Gan to kagaku ryoho. Cancer & chemotherapy.

[33]  R. Tothill,et al.  Epigenetic profiling to classify cancer of unknown primary: a multicentre, retrospective analysis. , 2016, The Lancet. Oncology.

[34]  L. Paz-Ares,et al.  Current Challenges in Cancer Treatment. , 2016, Clinical therapeutics.

[35]  M. Kriegsmann,et al.  Molecular driver alterations and their clinical relevance in cancer of unknown primary site , 2016, Oncotarget.

[36]  Melissa P. Murray,et al.  Massively parallel sequencing of phyllodes tumours of the breast reveals actionable mutations, and TERT promoter hotspot mutations and TERT gene amplification as likely drivers of progression , 2016, The Journal of pathology.

[37]  Ken R. Smith,et al.  Familial Risk in Patients With Carcinoma of Unknown Primary. , 2016, JAMA oncology.

[38]  J. Hainsworth,et al.  Lung Adenocarcinoma with Anaplastic Lymphoma Kinase (ALK) Rearrangement Presenting as Carcinoma of Unknown Primary Site: Recognition and Treatment Implications , 2016, Drugs - Real World Outcomes.

[39]  D. Visscher,et al.  Gene expression profiling identifies responsive patients with cancer of unknown primary treated with carboplatin, paclitaxel, and everolimus: NCCTG N0871 (alliance). , 2016, Annals of oncology : official journal of the European Society for Medical Oncology.

[40]  Richard B. Schwab,et al.  Detection rate of actionable mutations in diverse cancers using a biopsy-free (blood) circulating tumor cell DNA assay , 2016, Oncotarget.

[41]  P. Hou,et al.  TERT promoter mutations and long telomere length predict poor survival and radiotherapy resistance in gliomas , 2015, Oncotarget.

[42]  Nicolas Servant,et al.  Molecularly targeted therapy based on tumour molecular profiling versus conventional therapy for advanced cancer (SHIVA): a multicentre, open-label, proof-of-concept, randomised, controlled phase 2 trial. , 2015, The Lancet. Oncology.

[43]  P. Gibbs,et al.  Phase II Pilot Study of Vemurafenib in Patients With Metastatic BRAF-Mutated Colorectal Cancer , 2015, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[44]  J. Blay,et al.  Vemurafenib in Multiple Nonmelanoma Cancers with BRAF V600 Mutations. , 2015, The New England journal of medicine.

[45]  A. Chinnaiyan,et al.  Genomic Profiling of Cancers of Unknown Primary Site: The Next Steps. , 2015, JAMA oncology.

[46]  J. Hainsworth,et al.  Paclitaxel/carboplatin with or without belinostat as empiric first‐line treatment for patients with carcinoma of unknown primary site: A randomized, phase 2 trial , 2015, Cancer.

[47]  M. López-Lázaro,et al.  The migration ability of stem cells can explain the existence of cancer of unknown primary site. Rethinking metastasis , 2015, Oncoscience.

[48]  Kai Wang,et al.  Comprehensive Genomic Profiling of Carcinoma of Unknown Primary Site: New Routes to Targeted Therapies. , 2015, JAMA oncology.

[49]  J. Hainsworth,et al.  Poorly Differentiated Neoplasms of Unknown Primary Site: Diagnostic Usefulness of a Molecular Cancer Classifier Assay , 2015, Molecular Diagnosis & Therapy.

[50]  R. Tothill,et al.  Development and validation of a gene expression tumour classifier for cancer of unknown primary , 2015, Pathology.

[51]  V. Miller,et al.  A Poorly Differentiated Malignant Neoplasm Lacking Lung Markers Harbors an EML4-ALK Rearrangement and Responds to Crizotinib , 2014, Case Reports in Oncology.

[52]  Benjamin J. Raphael,et al.  Multiplatform Analysis of 12 Cancer Types Reveals Molecular Classification within and across Tissues of Origin , 2014, Cell.

[53]  D. Lipson,et al.  Durable Response to Crizotinib in a MET-Amplified, KRAS-Mutated Carcinoma of Unknown Primary , 2014, Case Reports in Oncology.

[54]  R. Celestino,et al.  TERT Promoter Mutations Are a Major Indicator of Poor Outcome in Differentiated Thyroid Carcinomas , 2014, The Journal of clinical endocrinology and metabolism.

[55]  David M. Thomas,et al.  Massively‐parallel sequencing assists the diagnosis and guided treatment of cancers of unknown primary , 2013, The Journal of pathology.

[56]  Benjamin J. Raphael,et al.  Mutational landscape and significance across 12 major cancer types , 2013, Nature.

[57]  Y. Lawrence,et al.  Cancer of unknown primary: a population-based analysis of temporal change and socioeconomic disparities , 2013, British Journal of Cancer.

[58]  A. Takano,et al.  Molecular profiling for druggable genetic abnormalities in carcinoma of unknown primary. , 2013, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[59]  N. Pavlidis,et al.  Exploring the biology of cancer of unknown primary: breakthroughs and drawbacks , 2013, European journal of clinical investigation.

[60]  Lynda Chin,et al.  Highly Recurrent TERT Promoter Mutations in Human Melanoma , 2013, Science.

[61]  D. Schadendorf,et al.  TERT Promoter Mutations in Familial and Sporadic Melanoma , 2013, Science.

[62]  J. Hainsworth,et al.  Molecular gene expression profiling to predict the tissue of origin and direct site-specific therapy in patients with carcinoma of unknown primary site: a prospective trial of the Sarah Cannon research institute. , 2013, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[63]  S. Yano,et al.  [Cancer of unknown primary site with epidermal growth factor receptor mutation for which gefitinib proved effective]. , 2012, Gan to kagaku ryoho. Cancer & chemotherapy.

[64]  S. Dry,et al.  Multisite Validation Study to Determine Performance Characteristics of a 92-Gene Molecular Cancer Classifier , 2012, Clinical Cancer Research.

[65]  N. Pavlidis,et al.  Cancer of unknown primary site , 2012, The Lancet.

[66]  S. Culine,et al.  Cisplatin alone or combined with gemcitabine in carcinomas of unknown primary: results of the randomised GEFCAPI 02 trial. , 2012, European journal of cancer.

[67]  Christophe Massard,et al.  Carcinomas of an unknown primary origin—diagnosis and treatment , 2011, Nature Reviews Clinical Oncology.

[68]  A. Hauschild,et al.  Improved survival with vemurafenib in melanoma with BRAF V600E mutation. , 2011, The New England journal of medicine.

[69]  K. Naresh,et al.  Angiogenic ability of metastatic squamous carcinoma in the cervical lymph nodes from unknown primary tumours , 2011, Journal of Clinical Pathology.

[70]  R. Weinberg,et al.  A Perspective on Cancer Cell Metastasis , 2011, Science.

[71]  K. Hemminki,et al.  Familial risks in cancer of unknown primary: tracking the primary sites. , 2011, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[72]  A. Bardelli,et al.  MET mutations in cancers of unknown primary origin (CUPs) , 2011, Human mutation.

[73]  M. Gilbert,et al.  Clinical Cancer Advances 2013: Annual Report on Progress Against Cancer from the American Society of Clinical Oncology. , 2010, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[74]  N. Pavlidis,et al.  Cancers of unknown primary site: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up. , 2010, Annals of oncology : official journal of the European Society for Medical Oncology.

[75]  J. Hainsworth,et al.  Paclitaxel/carboplatin plus bevacizumab/erlotinib in the first-line treatment of patients with carcinoma of unknown primary site. , 2009, The oncologist.

[76]  F. Monzon,et al.  Multicenter validation of a 1,550-gene expression profile for identification of tumor tissue of origin. , 2009, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[77]  P. Schőffski,et al.  Paclitaxel and carboplatin vs gemcitabine and vinorelbine in patients with adeno- or undifferentiated carcinoma of unknown primary: a randomised prospective phase II trial , 2008, British Journal of Cancer.

[78]  Kenneth R Hess,et al.  Molecular profiling of carcinoma of unknown primary and correlation with clinical evaluation. , 2008, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[79]  Arno Floore,et al.  Gene expression profiling to identify the histogenetic origin of metastatic adenocarcinomas of unknown primary. , 2008, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[80]  M. Dimopoulos,et al.  Multicenter phase-II trial of irinotecan plus oxaliplatin [IROX regimen] in patients with poor-prognosis cancer of unknown primary: a hellenic cooperative oncology group study , 2008, Cancer Chemotherapy and Pharmacology.

[81]  T. Economopoulos,et al.  Docetaxel and carboplatin combination chemotherapy as outpatient palliative therapy in carcinoma of unknown primary: A multicentre Hellenic Cooperative Oncology Group phase II study , 2008, Acta oncologica.

[82]  N. Pavlidis,et al.  Switching benchmarks in cancer of unknown primary: from autopsy to microarray. , 2007, European journal of cancer.

[83]  J. Hainsworth,et al.  Phase II trial of bevacizumab and erlotinib in carcinomas of unknown primary site: the Minnie Pearl Cancer Research Network. , 2007, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[84]  N. Pavlidis,et al.  Cancer of unknown primary site: missing primary or missing biology? , 2007, The oncologist.

[85]  R. Haba,et al.  Unknown primary carcinoma, diagnosed as inflammatory breast cancer,and successfully treated with trastuzumab and vinorelbine , 2005, International Journal of Clinical Oncology.

[86]  N. Pavlidis,et al.  Angiogenesis in cancer of unknown primary: clinicopathological study of CD34, VEGF and TSP-1 , 2005, BMC Cancer.

[87]  H. Hillen,et al.  The unknown biology of the unknown primary tumour: a literature review. , 2003, Annals of oncology : official journal of the European Society for Medical Oncology.

[88]  C. la Vecchia,et al.  Epidemiology of unknown primary tumours. , 2002, European journal of cancer.

[89]  R J Carroll,et al.  Phase II clinical trial design for noncytotoxic anticancer agents for which time to disease progression is the primary endpoint. , 2000, Controlled clinical trials.

[90]  E. Warner,et al.  A multicentre phase II study of carboplatin and prolonged oral etoposide in the treatment of cancer of unknown primary site (CUPS). , 1998, British Journal of Cancer.

[91]  K. Hess,et al.  Unknown primary carcinoma: natural history and prognostic factors in 657 consecutive patients. , 1994, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[92]  T. Chevalier,et al.  Early metastatic cancer of unknown primary origin at presentation. A clinical study of 302 consecutive autopsied patients. , 1988, Archives of internal medicine.

[93]  D. Hedley,et al.  Metastatic adeno or undifferentiated carcinoma from an unknown primary site--natural history and guidelines for identification of treatable subsets. , 1987, The Quarterly journal of medicine.

[94]  F. Holmes,et al.  Metastatic cancer of unknown primary site , 1970, Cancer.

[95]  Susan M. Chang,et al.  Clinical Cancer Advances 2019: Annual Report on Progress Against Cancer From the American Society of Clinical Oncology. , 2019, Journal of clinical oncology : official journal of the American Society of Clinical Oncology.

[96]  Matsumoto,et al.  Lung Cancer of Unknown Primary Site with EGFR Mutation as Indicated by Frozen Bone Specimen , 2016 .

[97]  M. Bissell Performance and Clinical Evaluation of the 92-Gene Real-Time PCR Assay for Tumor Classification , 2013 .

[98]  L. Buturovic,et al.  Validation and reproducibility of a microarray-based gene expression test for tumor identification in formalin-fixed, paraffin-embedded specimens. , 2011, The Journal of molecular diagnostics : JMD.

[99]  J. Coebergh,et al.  Epidemiology of unknown primary tumours; incidence and population-based survival of 1285 patients in Southeast Netherlands, 1984-1992. , 2002, European journal of cancer.

[100]  B. Lembersky,et al.  Metastases of unknown primary site. , 1996, The Medical clinics of North America.

[101]  C. Muir Cancer of unknown primary site , 1995, Cancer.

[102]  E. Cadman,et al.  An analysis of 1539 patients with cancer of unknown primary site , 1986, Cancer.