Tumor classification has historically relied primarily upon morphologic features identified by light microscopy. In the past decade, integration of high-throughput genomic testing into routine clinical workflows has refined the approach to diagnosing brain tumors. ¹ In this chapter, we explore tumor classification from traditional microscope-based approaches to currently available methodologies. We review genomic profiling and introduce the concept of an integrated diagnosis.

The chapter begins with a discussion of the histologic assessment of brain tumors, which is often the first data to be reported after a tumor surgery. This is followed by a discussion of molecular profiling, which is used to further classify these tumors, guide prognosis, and predict response to therapy. Molecular data typically returns in the weeks following surgery. Finally, we review a series of common case scenarios and integrate the histologic and molecular data into a final integrated diagnosis that clinicians can use to help manage and counsel these patients.

The process of converting a portion of resected brain tissue to an H&E stained section is the first step to achieve a tissue-based diagnosis. Brain tissues removed at the time of surgery can range from small biopsies, such as needle core biopsies, to large resections that often occur during a tumor debulking surgery. Once the fresh tissue reaches the laboratory, the sample is subjected to fixation in formalin-based solutions that serve to preserve tissues and cells.

Formalin-fixed tissues then undergo a series of steps, commonly referred to as tissue processing, which prepares the formalin-fixed tissues for embedding into a block of paraffin wax. Once the tissue fragment is embedded in paraffin and mounted into a cassette, this “block” serves as the final medium where the tissue can be safely stored for years (even decades). Importantly, this processing method preserves the integrity of the tissues for later use. Formalin-fixed paraffin-embedded (FFPE) samples are the mainstay of both traditional microscopic analysis and serve as the starting medium for most tissue-based molecular and genomic assays currently available.

Once a tissue sample is converted to an FFPE block, sections (5 microns thickness) can be cut from the block, placed onto glass slides, and subjected to staining with the dyes hematoxylin and eosin. Hematoxylin stains nucleic acids a deep blue-to-purple color, which readily highlights the nuclei of cells. Eosin stains other cellular components, like proteins, with a bright pink color that contrasts with the blue hematoxylin-stained nuclei—together these two dyes serve as the basis for all H&E-based tumor classification.

Brain tumor classification based on H&E features relies on the fact that the histologic appearance of these tumors is consistent from one patient to another. In fact, the features are so reproducible that they have been codified into the World Health Organization (WHO) Classification of Tumors of the Central Nervous System, which outlines the microscopic features present in all brain tumors and serves as the central resource to ensure all patients around the world are diagnosed and graded using the same criteria.

Tumor Grading. Unlike other tumors, which are staged based on size, lymph node involvement, and presence or extent of metastases (e.g., TNM classification), staging is not used for gliomas, which rarely spread beyond the central nervous system (CNS). Instead, gliomas are graded from grade I to IV and are broadly divided into low- and high-grade tumors. Grade I and II are considered “low grade” and grade III and IV as “high grade”; of these, grade I tumors are generally well circumscribed, whereas grades II–IV are diffusely infiltrating, albeit with some exceptions such as ependymoma and pleomorphic xanthoastrocytoma which tend to be well circumscribed despite conforming to grade II. The histologic features assessed to establish glioma grading include atypia, mitoses, endothelial or microvascular proliferation, and necrosis. Grade I tumors such as pilocytic astrocytomas are most commonly encountered in the pediatric setting. Although such tumors do occur in the adult population, the use of the term “lower-grade gliomas” in adults largely refers to infiltrating grade II tumors such as diffuse astrocytoma and oligodendroglioma. Grade III tumors include anaplastic astrocytoma (AA3) and anaplastic oligodendroglioma (AO3), whereas glioblastoma (GBM) is considered a grade IV astrocytoma. Progression of brain tumors from low to high grade does occur, most commonly in adul...