1 / 70

Clinicopathological Conference

Clinicopathological Conference. Nadia Nasreen , PGY 3 Resident UIUC IMRP. Chief Complaint. Chest pressure for one month progressively worsened for 2 days Weakness for 4 days Non-productive cough for 1 week. History of Presenting Illness.

sezja
Download Presentation

Clinicopathological Conference

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Clinicopathological Conference Nadia Nasreen, PGY 3 Resident UIUC IMRP

  2. Chief Complaint • Chest pressure for one month progressively worsened for 2 days • Weakness for 4 days • Non-productive cough for 1 week

  3. History of Presenting Illness • A 64y old Caucasian female with past medical history of hypertension and CAD went to outside hospital with chest pressure which has been going on for one month with worsening for 2 days. Pain was in middle of the chest, retrosternal, 4/10, no radiation or shift, no aggravating or relieving factors, associated with non-productive cough for last 1 week. • Negative for hemoptysis and weight loss.

  4. Past Medical and Surgical History • Hyperlipidemia, CAD, Hypertension • Appendectomy, Tonsillectomy, Nasal surgery • Medications • ASA, Atenolol, Allegra • Social History • 12 pack years, quit at 28yrs of age • Worked as spray painter in a boat manufacturing industry • No alcohol or drug use • FAMILY HX: • No hx of diabetes mellitus, pre-mature heart disease or cancers .

  5. Physical Exam • Temp: 97.9 F, Pulse : 81/min, Resp: 18/min , BP: 118/69, SpO2 : 99% on 2L • GEN: AO x 3, no distress • HEENT : Non-contributory • NECK: No JVD, No lymph-adenopathy • Chest: Non tender on palpation, clear on auscultation B/L • Heart : Normal heart sounds, No murmurs heard • Abdomen: Soft, non-tender, no organomegaly,BS+ • Extremities: No edema, DP + • Neuro: Non-focal exam • Skin: No rashes , echymosis or purpura

  6. Labs

  7. Labs

  8. Summary • 64 y/o caucasian female with PMH of HTN, CAD, presented with 1 month H/O retrosternal, non radiating 4/10, chest pressure, progressively worsening for last 2 days, weakness for 4 days, nonproductive cough for 1 week with no hemoptysis or weight loss. Remote H/O smoking , quit 36 years back and worked as a boat painter. • Lab- significant only for Mild normocytic anemia.

  9. Additional History Required • Comprehensive review of systems- Fever or chill, night sweat, anorexia. • Any Associated SOB, dysphagia, odynophagia , hoarseness • Pain with deep breathing or coughing • Description of weakness- Focal or generalized, vs any UE s/s- numbness/paresthesia • Axillary, inguinal supraclavicular lymph node examination • Any Breast examination for lump/mass • Lateral CXR to evaluate the mediastinal location.

  10. Imaging

  11. Lung vsMediastinal Mass • The following characteristics indicate that a lesion originates within the mediastinum: • Mediastinalmass will not contain air bronchograms. • Mediastinallines (azygoesophageal recess, anterior and posterior junction lines) will be disrupted. • There can be associated spinal, costal or sternal abnormalities. • A lung mass abutts the mediastinal surface and creates acute angles with the lung, while a mediastinal mass will sit under the surface creating obtuse angles with the lung

  12. Imaging

  13. Imaging

  14. Differential Diagnoses • Bronchogenic Carcinoma • Primary Lung cancer NSCLC vs SCLC • Metastatic neoplasms to Lungs • Sarcomatoid carcinoma • Lymphoproliferative disorders • NHL • Hodgkins lymphoma • Primary mediastinal large B cell Lymphoma • Primary Pulmonary Lymphoma • Extramedullaryplasmacytoma (primary pulmonary plasmacytoma) • Lymphomatoidgranulomatosis • Postobstructive pneumonia • Viral or bacterial pneumonia • Atypical/ Chronic Infections- • Pulmonary TB • Fungal – • Histoplasmosis • Aspergillosis, • Blastomycosis • Cryptococcal • coccidioidimycosis • Bronchial Carcinoid • Sarcoidosis • Collagen vascular disease- GPA( Wegners), SLE, RA • Asbestos associated Lung disease • Mediastinal involvement( Mainly posterior) • Esophageal Carcinoma • Neurogenic tumors- Schwannomas, meningocele, paraspinalGanglioneuroma

  15. Bronchogenic Carcinoma • Lung cancer is the leading cause of cancer death in the United States, accounting for approximately 29% of all cancer deaths. • lung cancer is the second most common cancer in man and women • During 2008, approximately 213,380 new cases of lung cancer were diagnosed (114,760 among men and 98,620 among women).

  16. Epidemiology • Age Distribution-predominately in persons aged 50-70 years. • Nearly 70% of patients are older than 65 years and fewer than 3% are younger than 45 years. • Sex- In the United States, the probability of developing lung cancer remains equal in both sexes until age 39 years It then starts to increase among men compared with women, reaching a maximum in those older than 70 years. • Prevalence-incidence rates are similar among African American and white women. • Approximately 45% higher among African American men than among white men • Current 5-year survival rates are estimated to be 16% among whites and 13% among non-whites

  17. Etiology • Causes: • Smoking (90% of all Lung cancers)- • The risk of developing lung cancer for a current smoker of 1 ppd for 40 years is approximately 20 times that of someone who has never smoked. • Risk declines slowly after smoking cessation. The relative risk remains high in the first 10 years after cessation and gradually declines to 2-fold approximately 30 years after cessation. • Asbestos exposure- risk of Lung cancer is 5 times. Synergistic with smoking- 80-90 times greater risk than control population

  18. Environmental toxins • - Radon , halogen , ether, arsenic atmospheric pollution • Chromium, nickel , Vinyl chloride • Radiation therapy —increase the risk of a second primary lung cancer in patients who have been treated for other malignancies. • Pulmonary fibrosis —The risk for lung cancer is increased about sevenfold patients with pulmonary fibrosis, Independent of Smoking • HIV infection — The incidence among individuals infected with HIV appears to be increased compared to that seen in uninfected controls • Genetic Exposure-. The ras gene mutations occur almost exclusively in adenocarcinoma and are found in 30% of such cases. • mutations in c-myc and c-raf among oncogenes and retinoblastoma (Rb) and p53 among tumor suppressor gene are found in NSCLC include

  19. Classification Lung Cancer Small Cell Lung cancer- 10%-15%of Lung cancers Non-small Cell Cancer- 85%-90% of Lung cancers • Adenocarcinoma((including bronchioloalveolar carcinoma) — 38 percent • Squamous cell carcinoma — 20 percent • Large Cell Carcinoma - 5% • Other non-small cell carcinomas - • cannot be further classified (18 percent) • Others- Sarcomatoid, NE tumors- 6%

  20. Adenocarcinoma • Adenocarcinoma, arising from the bronchial mucosal glands • The most frequent NSCLC in the United States, -35-40% of all lung cancers. • It usually occurs in a peripheral location within the lung. • Adenocarcinoma is the most common histologic subtype, and may manifest as a “scar carcinoma.” most commonly in persons who do not smoke. This type may manifest as multifocal tumors in a bronchoalveolar form. • Significant variation in architecture of neoplastic gland formation. • Variant Subtypes: - Acinar - Papillary - Bronchiloalveolar Carcinoma - Solid Adenocarcinoma with mucin production

  21. Bronchiloalveolar Carcinoma • Bronchoalveolar carcinoma is a distinct subtype of adenocarcinoma with a classic manifestation as an interstitial lung disease on chest radiograph. • Bronchoalveolar carcinoma arises from type II pneumocytes and grows along alveolar septa. This subtype may manifest as a solitary peripheral nodule, multifocal disease, or a rapidly progressing pneumonic form. A characteristic finding in persons with advanced disease is voluminous watery sputum. • In the new classification scheme, these tumors have been renamed as adenocarcinoma in situ • has a propensity for intrapulmonary metastases and a more indolent course

  22. Squamous Cell Carcinoma • 25-30% of all lung cancers. • Tends to occur centrally, with endobronchial lesions • Histologically : presence of keratin pearls detected with cytologic studies and has a tendency to exfoliate. It is the type most often associated with hypercalcemia. • Historically, most squamous cell carcinoma (60 to 80 percent) arose in the proximal portions of the tracheobronchial tree • A minority of cases occur peripherally and may be associated with bronchiectatic cavities or scars.Central and peripheral squamous cell carcinomas may show extensive central necrosis with resulting cavitation • The classic manifestation is a cavitary lesion in a proximal bronchus.

  23. Large Cell Undifferentiated Carcinoma • only 10% of lung cancers. • Typically manifest as a large peripheral mass on chest radiograph • Histologically, this type has sheets of highly atypical cells with focal necrosis, with no evidence of keratinization (typical of SCC) or gland formation (typical of adenocarcinomas). • LCC is a diagnosis of exclusion intended to include all poorly differentiated NSCLCs that are not further classifiable by routine light microscopy.

  24. Sarcomatoid Carcinoma • Represents a heterogeneous group of NSCLCs that contain a component of sarcoma or sarcoma-like elements: • Pleomorphic carcinoma • Spindle cell carcinoma • Giant cell carcinoma • Carcinosarcoma —defined by the presence of a typical carcinoma combined with sarcomatous elements (bone, cartilage or skeletal muscle). Typical sarcomatous components include rhabdomyosarcoma, osteosarcoma, and chondrosarcoma. • Pulmonary blastoma —biphasic malignancies that have an adenocarcinoma component that has the appearance of fetal adenocarcinoma and a stroma that resembles that seen in Wilms tumor. They are usually large at the time of presentation and are highly malignant

  25. Pulmonary Neuroendocrine Tumors • Small cell carcinoma • large cell neuroendocrine carcinoma • Typical carcinoid, and atypical carcinoid • DIPNH- diffuse idiopathic pulmonary neuroendocrine cell hyperplasia, a possibly preinvasive epithelial lesion • Typical and atypical carcinoids - similar to carcinoid lesions arising at other sites. • Small cell carcinomas and large cell neuroendocrine carcinomas more aggressive course and pathologically by a much higher mitotic activities.

  26. Small Cell Lung Cancer • Small cell lung carcinoma (SCLC) accounts for approximately 15 percent of all bronchogenic carcinomas. • SCLC shows a strong correlation(>95%) with cigarette smoking and is extremely rare in persons who have never smoked. • SCLC is usually more aggressive than NSCLC . • Presents as a central lesion with hilar and mediastinal invasion along with regional adenopathy. • 65-70% of patients with SCLC have disseminated or extensive disease at presentation • The most common sites of metastasis of lung cancer are the bones, liver, adrenal glands, pericardium, brain, and spinal cord. • production of various peptide hormones leads to a wide range of paraneoplastic syndromes

  27. Clinical presentations

  28. Paraneoplastic Syndromes from lung cancers: • Hypercalcemia- Squamous cell carcinoma • Trousseau syndrome- Adenocarcinoma • Hypertrophic pulmonary osteoarthropathy- NSCLC • Clubbing – all types.

  29. Paraneoplastic Syndromes Of SCLC

  30. Diagnostic Imaging • CXR- may show the following: • Pulmonary nodule, mass, or infiltrate • Mediastinal widening • Atelectasis • Hilar enlargement • Pleural effusion • CT Scan -mediastinal lymphadenopathy. CT had a pooled sensitivity of 57%, a specificity of 82%, and a negative predictive value of 83%. • PET FDG- pooled sensitivity of 84% and a specificity of 89%, with a PPV of 79% and a NPV of 93%. • Combined positive predictive value and negative predictive value of CT scanning and PET-FDG were 83% to 93% and 88% to 95%, respectively. • PET-FDG is superior to CT scanning in the staging of disease in patients with mediastinal lymph node involvement.

  31. Staging of SCLC • TNM system is generally not used in these patients. • The Veterans Administration Lung Study Group staging system is typically used, : as limited or extensive. • Limited-stage disease -limited to one hemithorax, with hilar and mediastinal lymphadenopathy that can be encompassed within one tolerable radiotherapy portal. • Extensive-stage disease consists of any disease that exceeds those boundaries. Most patients (60% to 70%) with SCLC present with clinically extensive-stage disease. significant differences in median and 5-year survival among these patients depending on the stages. Combination chemotherapy is the cornerstone of treatment for both limited-stage and extensive-stage SCLC.

  32. Metastatic Neoplasm to Lungs • Approximately 10-30% of all malignant nodules resected from the lung are metastatic • Frequent sources of malignancy: • Head and neck • Colon • Kidney • Breast • Thyroid gland • Melanoma • In addition to solitary or multiple nodules, metastases of carcinoma to the lung include lymphangiitic, endobronchial, pleural, and embolic patterns. • Most common Clinical situation: multiple or innumerable nodules.

  33. Lymphomatous proliferation involving Lungs • 3 different ways: • Haematogenousdissemination of Non-Hodgkinslymphoma (NHL) or Hodgkins disease • Contiguous invasion from a hilaror mediastinalsite of nodal lymphoma • Primary pulmonary involvement.

  34. Non-Hodgkins Lymphoma • Epidemiology- Approximately 56,000 new cases (NHL) are diagnosed in the United States annually, with approximately 24,000 people dying from this disease each year. • The incidence of NHL increases exponentially with age and is greater in men than women and in whites than blacks. • Risk Factors: • Autoimmune disease and immunodeficiency states have a known association with NHL. • NHL may also be caused by viruses – EBV- Burkitts lymphoma, HTLV-1- Adult T cell leukemia- lymphoma, HHV-8- Body cavity lymphoma • Several chemicals, such as organochlorine agents (for example, DDT), have been weakly associated with an increased risk for NHL. • Farming - consistently shows an association with an increased risk for NHL, which is often thought to be related to the use of pesticides

  35. WHO Classification Of Lymphoid Malignancy Lymphoid Neoplasms B cell neoplasms T- cell and NK -cell neoplasms Hodgkins Lymphoma Classification Criteria: Morphology Clinical features Genetic features Immunophenotype

  36. 80%-85% of NHL in adults are B-cell in origin • Remainder – mostly T cell in origin • B cell Lymphomas- based on biology and natural history: • Indolent vs Aggressive vs Highly aggressive Groups

  37. Clinical presentations • Aggressive NHLs - • acutely or subacutely with a rapidly growing mass, systemic B symptoms (ie, fever, night sweats, weight loss), and/or elevated levels of serum LDH and uric acid • 50% present with secondary extranodal disease, 10%-35% Primary extranodal lymphoma • - Most common EN site- GI tract then skin. Others – Testis, Bone, Kidney • potentially are curable with combination chemotherapy. • Indolent lymphomas • Are often insidious, presenting only with slow growing lymphadenopathy, hepatomegaly, splenomegaly, or cytopenias.. • Mostly present at advanced stage, incurable • Median survival 7-10years.

  38. Chest and Lung NHL • Approximately 20 percent of patients with NHL present with mediastinaladenopathy on clinical examination or chest radiograph • Primary mediastinal large B cell lymphoma or part of diffuse Systemic disease • Cough, chest discomfort, or asymptomatic with abnormal CXR • 3%-8%- SVC syndrome • Other - include pleural and, less commonly, pericardial effusions. Chylothorax, alone or in combination with chylopericardium or chylousascites • Pleural disease is seen in up to 10 percent of all patients with NHL at diagnosis.

  39. PA (upper panel) and lateral (lower panel) radiographs of a patient with a large right-sided mediastinal mass (arrows). The biopsy was consistent with diffuse large B-cell non-Hodgkin's lymphoma.

  40. CT scan of Chest in NHL • Typical radiographic findings include alveolar opacities (consolidation, masses, or nodules) and peribronchialdisease. • parenchymal lung lesions can be seen with no evidence of mediastinal or hilar lymphadenopathy. Diagnosis: NCCN recommends- An excisional biopsy of an intact node - histologic, immunologic, and molecular biologic assessment Including flow cytometry and fluorescent in-situ hybridization or cytogenetics. Staging- CT chest abdomen, pelvis, PET scan, CBC, CMP, LDH, , Uric acid, BM Bx, Lumber puncture, Echocardiogram, NM scan

  41. Diffuse Large B Cell Lymphoma • Most common Lymphoid malignancy. 25% of NHL • Caucasian Americans having higher rates than Blacks, Asians, and American Indian or Alaska Natives • male predominance ;approximately 55 percent of cases in men • Median age at presentation is 64 years. Younger for Blacks. • Typically presents as rapidly enlarging symptomatic mass, nodal enlargement- usually neck and abdomen • B-symptoms- 30% • BM – 30%, Extramedullary- 40% • tumors derived from germinal center B cells or post-germinal center B cells (also called activated B cells) • majority of DLBCL tumors demonstrate translocations or mutations that result in the increased expression of the B cell lymphoma 6 (BCL-6) gene.

  42. Hodgkins Lymphoma • Arises from germinal or post-germinal center B cells. • Incidence- approximately 10 percent of all lymphomas in economically advanced countries. • Age and sex- Bimodal distribution- 1 peak in young adults (age 20 years) and one in older age (age 65 years); the majority of patients are young adults; male predominance • Based on the appearance and immunophenotype of the tumor cells: • Nodular lymphocyte predominant HL (NLPHL) • Classical HL • Classic HL is usually diagnosed by lymph node biopsy. • On light microscopy, the tumor contains a minority of neoplastic cells (Reed-Sternberg cells and their variants) in an inflammatory background. • The neoplastic cells typically express CD15 and CD30, variably express CD20, and do not express CD3 or CD45

  43. Classical HL is further divided into the following four subtypes: • Nodular sclerosis classical HL • Mixed cellularity classical HL • Lymphocyte rich classical HL • Lymphocyte depleted classical HL • Clinical presentations include • Nontender lymphadenopathy in the neck or mediastinum • Incidental finding of a mediastinal mass on routine chest x-ray • Systemic symptoms - in less than 20 percent of stage I/II Hodgkin lymphoma • up to 50 percent of patients with more advanced disease. • Nonspecific symptoms- retroperitoneal LAD, cholestatic liver disease, alcohol-induced pain, skin lesions, neurologic symptoms, nephrotic syndrome, hypercalcemia, and abnormalities in blood counts. • Spread- via lymphatic channels before disseminating to distant nonadjacent sites and organs. • It is uncommon to have pulmonary disease at presentation without Hodgkin lymphoma being present within the hilar lymph nodes, usually on the ipsilateral side

  44. Primary Pulmonary Lymphoma (PPL) • clonal lymphoid proliferation affecting one or both lungs (parenchyma and/or bronchi) in a patient with no detectable extrapulmonary involvement at diagnosisor during the subsequent 3 months • PPL is very rare; 0.5–1% of primary pulmonary malignancies, <1% of NHL • The current definition of PPL covers: • 1) lowgrade B-cell PPL (PPL-B), the most frequent form • 2) high-grade PPL-B • 3) lymphomatoidgranulomatosis(LG), a rare disorder.

More Related