Neural stem cells (NSCs) intrinsically migrate to sites of brain tumors, and engineered NSCs offer a promising mechanism for local delivery of therapeutic agents. While many groups have observed that therapeutically modified NSCs migrate selectively to glioma foci, quantitative assessments of NSC migration efficiency and local distribution at tumor sites, as well as tumor coverage estimated for the therapeutics delivered by these NSCs, have been difficult to perform. In this article, we present a quantitative analysis of immunostained serially sectioned formalin-fixed paraffin-embedded (FFPE) brain tissue across multiple test animals, thereby providing a paradigm facilitating optimization of this and other cell-based therapies.