Multiple Primary Lung Cancer (MPLC) is increasingly diagnosed in clinical practice and is classified as synchronous MPLC (sMPLC) and metachronous MPLC (mMPLC). Differentiating MPLC from intrapulmonary metastases (IPM) is paramount in the selection of optimal therapeutic approaches. Distinguishing is based on histological, imaging, and molecular evaluation, and molecular diagnostics has transformed precision in the diagnosis of MPLC. Surgery is still the main treatment, with stereotactic radiotherapy and ablation reserved for inoperable diseases. Targeted treatment and immunotherapy provide hope for certain patients, highlighting the necessity of a multi-disciplinary system. Refinement of diagnostic standards, establishment of standardized treatment regimens, and optimization of molecular profiling methods need to be further researched to provide better outcomes for patients.
Lung cancer continues to be the main cause of cancer death globally. Multiple Primary Lung Cancer (MPLC), comprising synchronous (sMPLC) and metachronous (mMPLC) types, is increasingly common with better diagnostic tools and increased survival in patients with lung cancer. The differentiation of MPLC from intrapulmonary metastases (IPM) is an essential problem of thoracic oncology. With improvements in imaging modalities, histopathological methods, and molecular analysis, the accuracy in diagnosing and treating MPLC has improved considerably. This article discusses the recent advances in the diagnosis and management of MPLC with a focus on a multidisciplinary approach.
MPLC is classified into:
Synchronous MPLC (sMPLC) – Defined as two or more primary lung tumors diagnosed simultaneously or within six months of the initial cancer diagnosis.
Metachronous MPLC (mMPLC) – Refers to lung tumors developing at different time intervals, usually more than six months apart.
Unlike IPM, where a single primary tumor gives rise to metastatic lesions, MPLC represents independent neoplastic processes with distinct genetic and histopathological profiles. This distinction is critical for determining prognosis and guiding treatment decisions.
Imaging Modalities
Computed Tomography (CT) and Positron Emission Tomography (PET-CT): CT scans provide detailed anatomical visualization, while PET-CT enhances metabolic differentiation between benign and malignant lesions.
Magnetic Resonance Imaging (MRI): Occasionally used to assess mediastinal invasion and brain metastases in MPLC cases.
Histological Assessment
Biopsy and histopathological examination are essential for distinguishing separate primary tumors from metastatic disease.
The use of immunohistochemical markers aids in identifying tumor origin and differentiation.
Molecular and Genetic Profiling
Next-Generation Sequencing (NGS) has revolutionized MPLC diagnosis by providing insights into genetic mutations, aiding in tumor differentiation and targeted therapy selection.
Common genetic alterations in MPLC include mutations in EGFR, KRAS, and TP53, distinguishing them from metastatic tumors originating from a single clone.
Surgical Management
Lobectomy and Sublobar Resection: Surgical resection is the preferred treatment for MPLC when feasible. Lobectomy is the gold standard, but sub lobar resection (segmentectomy or wedge resection) may be considered for patients with limited lung function.
Minimally Invasive Surgery: Video-assisted thoracoscopic surgery (VATS) and robotic-assisted techniques have improved post-operative recovery and reduced morbidity.
Radiotherapy
Stereotactic Body Radiotherapy (SBRT): A non-invasive option for patients ineligible for surgery, delivering high-dose, focused radiation to tumor sites with minimal damage to surrounding tissue.
Intensity-Modulated Radiotherapy (IMRT): Allows precise dose distribution, minimizing toxicity while maximizing tumor control.
Systemic Therapy
Targeted Therapy:
EGFR inhibitors (e.g., osimertinib) for EGFR-mutated tumors.
ALK inhibitors (e.g., alectinib) for ALK-positive MPLC.
Immunotherapy:
Immune checkpoint inhibitors (e.g., pembrolizumab, nivolumab) are being explored as potential treatment options for MPLC, particularly in tumors with high PD-L1 expression.
Chemotherapy: Platinum-based regimens remain the standard for patients ineligible for targeted therapies.
Given the multitude of variables in MPLC, multidisciplinary team (MDT) management is crucial, and this includes pulmonologists, thoracic surgeons, medical oncologists, radiation oncologists, and pathologists. MDT meetings maximize individualized planning by combining diagnostic reports, patient choice, and changing therapeutic options.
Standardizing Diagnostic Criteria
Current diagnostic algorithms lack universal consensus on distinguishing MPLC from IPM. Developing standardized guidelines incorporating molecular and imaging data is crucial.
Refining Treatment Algorithms
With evolving molecular classifications, tailoring treatment regimens based on genetic and histological characteristics will improve patient outcomes.
Advancing Molecular Profiling
Expanding the use of NGS and liquid biopsy techniques will facilitate early detection and real-time monitoring of tumor evolution.
Long-Term Surveillance Strategies
Given the risk of recurrence in MPLC patients, robust follow-up protocols incorporating serial imaging and biomarker assessments are needed to detect new primary tumors early.
MPLC is a separate clinical entity that necessitates accurate differential diagnosis from IPM. Technical advances in imaging, histology, and molecular diagnostics have enhanced the accuracy of the classification of MPLC, allowing more targeted treatment regimens. Surgery is the mainstay of treatment, but radiotherapy, targeted therapy, and immunotherapy provide effective alternatives for unresectable diseases. Optimizing patient care requires multidisciplinary management. Future studies should aim at standardization of diagnostic criteria, optimization of treatment modalities, and utilization of molecular findings to improve prognosis and therapeutic response. Through the integration of these developments, the treatment of MPLC will continue to change, ultimately leading to better patient outcomes with this multifaceted disease process.
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