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Diffusivity Measurements Differentiate Benign from Malignant Lesions in Patients with Peripheral Neuropathy or Plexopathy
Authors:EL Yuh  S Jain Palrecha  GM Lagemann  M Kliot  PR Weinstein  NM Barbaro  CT Chin
Abstract:BACKGROUND AND PURPOSE:Peripheral nerve disorders caused by benign and malignant primary nerve sheath tumors, infiltration or compression of nerves by metastatic disease, and postradiation neuritis demonstrate overlapping features on conventional MR imaging but require vastly different therapeutic approaches. We characterize and compare diffusivities of peripheral nerve lesions in patients undergoing MR neurography for peripheral neuropathy or brachial or lumbosacral plexopathy.MATERIALS AND METHODS:Twenty-three patients, referred for MR neurography at our institution between 2003 and 2009 for a peripheral mononeuropathy or brachial or lumbosacral plexopathy and whose examinations included DWI, received a definitive diagnosis, based on biopsy results or clinical and imaging follow-up, for a masslike or infiltrative peripheral nerve or plexus lesion suspicious for tumor. Mean ADC values were determined within each lesion and compared across 3 groups (benign lesions, malignant lesions, and postradiation changes).RESULTS:Both ANOVA and Kruskal-Wallis tests demonstrated a statistically significant difference in ADC values across the 3 groups (P = .000023, P = .00056, respectively). Post hoc pair-wise comparisons showed that the ADC within malignant tumors differed significantly from that within benign tumors and postradiation changes. ADC within benign tumors and postradiation changes did not differ significantly from each other.CONCLUSIONS:DWI may be highly effective for the differentiation of benign from malignant peripheral nerve masslike or infiltrative lesions.

Peripheral neuropathies can be divided into mononeuropathies, polyneuropathies, and plexopathies. Patients present with pain, sensory symptoms, and/or motor deficits in the distribution of a single peripheral nerve, multiple peripheral nerves, or a nerve plexus. Mononeuropathies affect a single peripheral nerve. Polyneuropathies affect multiple peripheral nerves. In plexopathies, symptoms are localized to the brachial or lumbosacral plexus.Polyneuropathies are generally attributable to systemic diseases (eg, diabetes and vitamin deficiencies), while mononeuropathies are most often due to trauma, nerve compression syndromes that occur at a few characteristic anatomic locations, or mass lesions. History and physical examination, supplemented in a subset of cases by laboratory studies, electrodiagnostic studies, and neuroimaging, are the main tools for diagnostic evaluation. In patients with a classic compression mononeuropathy, such as median nerve compression at the carpal tunnel, the diagnosis can often be made clinically and corroborated by needle electromyography, nerve conduction, and/or imaging studies.14 For mononeuropathies involving nerves not typically susceptible to compression syndromes, imaging can play an essential role in identifying the lesion and guiding management.Plexopathies give rise to motor and/or sensory deficits in an extremity. Most brachial plexopathies (75%) are attributable to postradiation changes, primary and metastatic lung cancer, or metastatic breast cancer.5 Common causes of lumbosacral plexopathy are primary and metastatic tumor, including cervical, endometrial, ovarian, prostate, testicular, and colorectal cancer; postradiation changes; and diabetes.6 For patients with a history of radiation for malignancy, recurrent tumor with nerve invasion must be distinguished from radiation plexopathy; both can develop months to years following therapy and can have similar clinical presentations.6Although benign and malignant primary nerve sheath tumors, infiltration of nerves by metastatic disease, and postradiation neuritis require different therapeutic approaches, they also demonstrate overlapping features on MR imaging, including T2 hyperintensity, focal enlargement, and enhancement.7,8 Diffusivity measurements from DWI may be helpful in differentiating distinct pathologic entities. In prior studies, DWI was useful in differentiating malignant and benign peripheral nerve sheath tumors,9 retroperitoneal masses,10 head and neck tumors,11,12 and lymph nodes.13,14 Other studies have demonstrated differences in the diffusivities of adult15 or pediatric brain tumors16 that correlate with tumor grade and/or histologic type. In this study, we focus on masslike or infiltrative lesions of the peripheral nerves detected by MR imaging in patients presenting clinically with a peripheral mononeuropathy or plexopathy. We characterize and compare the diffusivities of these lesions and demonstrate significant differences among benign and malignant peripheral nerve tumors and postradiation changes.
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