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Home » Seasonal Allergies

Consultant. Vol. 49 No. 9
Photoclinic
Foresee Your Next Patient 

Large B-Cell Lymphoma

By ROBERT ZAIDEN, MD, TIMMY NGUYEN, MD, and FAUZIA RANA, MD
University of Florida Health Science Center, Jacksonville | September 11, 2009

Progressively worsening nasal congestion and headaches with diplopia and left proptosis for 2 months prompted an ophthalmology consultation for a 67-year-old woman. She had been evaluated multiple times for allergic rhinitis and recurrent sinusitis.

The patient had moderate proptosis; extraocular motions of the left eye were restricted in all directions. She had no lymphadenopathy. Oropharynx was visually unremarkable; however, fiberoptic nasopharyngoscopy revealed a posterior superior nasal cavity mass. A contrast CT scan of the head showed a large mass lesion at the level of the ethmoid sinus, eroding into the left orbit and displacing the left globe (A).

MRI of the head showed a 5.3 x 4.2 x 4.2-cm enhancing mass at the base of the brain that extended into the nasal cavity, with erosion into the cribriform plate, ethmoid sinuses, and planum sphenoidale. Results of an ethmoid sinus mass biopsy confirmed high-grade diffuse large B-cell lymphoma. Staging CT scans showed no metastatic disease, and cerebrospinal fluid analysis revealed no malignant cells. A bone marrow biopsy specimen showed no evidence of light chain monoclonality, no overt evidence of B-cell lymphoproliferative disorder on flow cytometry analysis, and no lymphoma. This was consistent with stage IAE disease.

Paranasal and sinus cavity lymphomas are rare presentations of extranodal disease; they represent fewer than 0.2% of all malignant lymphomas1 and only 1.5% of non- Hodgkin lymphomas.2 They usually go unrecognized until advanced symptomatic presentations.

Sinonasal lymphomas are either of B- or T-cell histology; the former represent most cases in the Western Hemisphere. B-cell sinonasal lymphomas usually occur in the sinus cavities, where nasal obstruction and discharge, unilateral facial swelling, and pain are frequent early manifestations. T-cell sinonasal lymphomas are more often found in the nasopharynx, typically with more inflammation, fibrosis, necrosis, and vascular invasion. The most common cause of death is disseminated disease, 3 which is more likely in patients with systemic symptoms, such as fever, malaise, night sweats, and weight loss.

Combined chemotherapy and region-specific consolidation radiation therapy followed by intrathecal chemoprophylaxis, typically with methotrexate(Drug information on methotrexate) and/or cytarabine(Drug information on cytarabine), provides the best chance for overall survival, because this aggressive type of lymphoma poses a direct threat to the skull base and brain. The cure rates are 68% to 82%, similar to those of localized large cell lymphomas in more common sites.4,5 The strongest predictor of outcome is extent of disease at diagnosis, with CNS dissemination common in later stages.

In this patient, treatment with R-CHOP chemotherapy for 6 cycles resulted in excellent clinical and radiological response (B).

 

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REFERENCES:
1. Fellbaum C, Hansmann ML, Lennert K. Malignant lymphomas of the nasal cavity and paranasal sinuses. Virchows Arch A Pathol Anat Histopathol. 1989;414:399-405.

2. Frierson HF Jr, Mills SE, Innes DJ Jr. Non- Hodgkin’s lymphomas of the sinonasal region: histologic subtypes and their clinicopathologic features. Am J Clin Pathol. 1984;81:721-727.

3. Proulx GM, Park J, Wang CC. Treatment of non-Hodgkin’s lymphoma of the nasal cavity and paranasal sinuses with radiation alone or in combination with chemotherapy or surgery. Int J Radiat Oncol Biol Phys. 1997;39(2 suppl 1).

4. Connors JM. Problems in lymphoma management: special sites of presentation. Oncology (Williston Park). 1998;12:185-195.

5. Fisher RI, Gaynor ER, Dahlberg S, et al. Comparison of a standard regimen (CHOP) with three intensive chemotherapy regimens for advanced non- Hodgkin’s lymphoma. N Engl J Med. 1993;328: 1002-1006.


 
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