Integrated Molecular and Clinical Characterization of Pulmonary Large Cell Neuroendocrine Carcinoma

  1. Anne Chiang
  2. Amin Nassar
  3. Chul Kim
  4. Tolulope Adeyelu
  5. Elias Farhat
  6. Hassan Abushukair
  7. Mehrdad Rakaee
  8. Kelsey Matteson
  9. Shun-Fat Lau
  10. Jesus Antonio Ocejo Gallegos
  11. Fatemeh Ardeshir-Larijani
  12. Ticiana Leal
  13. Suresh Ramalingam
  14. Sumaye Alam
  15. Jhanelle Gray
  16. James Hicks
  17. David Kaldas
  18. Javier Baena
  19. Maria Zurera Berjaga
  20. Frank Aboubakar Nana
  21. Christian Grohé
  22. Heike Leuders
  23. Fabrizio Citarella
  24. Alessio Cortellini
  25. Emanuele Claudio Mingo
  26. Danny Pancirer
  27. Millie Das
  28. Timothy Ellis-Caleo
  29. Justin Cheung
  30. Jessica Lin
  31. Alexander Watson
  32. D. Ross Camidge
  33. Arthi Srid
  34. Kaushal Parikh
  35. Fionnuala Crowley
  36. Thomas Marron
  37. Vanya Aggarwal
  38. Murtaza Ahmed
  39. Kamya Sankar
  40. Hassan Kawtharany
  41. Jun Zhang
  42. Dwight Owen
  43. Mingjia Li
  44. Misako Nagasaka
  45. David Pinato
  46. Nichola Awosika
  47. Khaled Alhamad
  48. Sonam Puri
  49. Unaiza Zaman
  50. Divya Gupta
  51. Chelsea Lau
  52. Hina Khan
  53. Justin Liauw
  54. Ana Velazquez
  55. Tyiesha Brown
  56. Laura Moliner
  57. Miguel Mosteiro
  58. Pedro Rocha
  59. Mark Evans
  60. Ari Vanderwalde
  61. Andrew Elliott
  62. Jorge Nieva
  63. Gilberto Lopes
  64. Patrick C Ma
  65. Hossein Borghaei
  66. Matthew Lee
  67. Lauren Young
  68. Raid Aljumaily
  69. Haris Mirza
  70. David Kwiatkowski
  71. Roy Herbst
  72. Richard Flavell
  73. Abdul Rafeh Naqash
  74. Yamato Takebe
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Abstract

Pulmonary large cell neuroendocrine carcinoma (LCNEC) is a rare, aggressive lung tumor marked by significant molecular heterogeneity. In a study of 590 patients across two independent cohorts, we observed comparable overall survival across treatment regimens (chemotherapy, chemoimmunotherapy, immunotherapy) without unexpected adverse events. Genomic analysis identified distinct NSCLC-like (KEAP1, KRAS, STK11 mutations) and SCLC-like (RB1, TP53 mutations) LCNEC subtypes, with 80% aligning with SCLC transcriptional profiles. Serial sampling revealed stable mutational but shifting transcriptomic landscapes over time. NSCLC-like LCNECs showed elevated FGL-1 (a LAG-3 ligand) and SPINK1 expression, while SCLC-like subtypes expressed higher levels of DLL3. Immunofluorescence confirmed FGL-1 in NSCLC-like LCNECs, and H&E slide analyses indicated fewer tumor-infiltrating lymphocytes in LCNECs versus other lung cancers. These findings highlight LCNEC’s distinct immunogenomic profile, supporting future investigations into LAG-3, SPINK1, and DLL3-targeted therapies.

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