Neural transplants in patients with Huntington's disease undergo disease-like neuronal degeneration

Abstract: The clinical evaluation of neural transplantation as a potential treatment for Huntington's disease (HD) was initiated in an attempt to replace lost neurons and improve patient outcomes. Two of 3 patients with HD reported here, who underwent neural transplantation containing striatal anlagen in the striatum a decade earlier, have demonstrated marginal and transient clinical benefits. Their brains were evaluated immunohistochemically and with electron microscopy for markers of projection neurons and interneuron… Show more

“…Yet medial ganglionic eminence components are also important for both the proper development of striatal structures, and for their functional integration [25]. This may explain, at least in part, the lack of functional integration in the clinical trial reported by Hauser et al [13], in which the grafts only consisted of the most lateral part of the lateral ganglionic eminence [13,26].…”

Cellular Therapy and Induced Neuronal Replacement for Huntington's Disease

“…Yet medial ganglionic eminence components are also important for both the proper development of striatal structures, and for their functional integration [25]. This may explain, at least in part, the lack of functional integration in the clinical trial reported by Hauser et al [13], in which the grafts only consisted of the most lateral part of the lateral ganglionic eminence [13,26].…”

Cellular Therapy and Induced Neuronal Replacement for Huntington's Disease

“…However, an immune reaction has been observed at least in some cases. Recent studies have shown either the presence of anti-HLAs or inflammation [22,[105][106][107]. Krystkowiak et al [107] reported that as many as half of the HD patients had immunization develop against donor antigens during their phase II multi-center study of fetal neural transplants, with 1 patient showing full clinical, radiological, and biological symptoms of immune rejection.…”

“…This function is highly dependent on the integrity of striatal neural networks, in particular the fronto-striatal circuitry [19,20]. In the few transplanted patients autopsied, histological analyses at 18 months [21] to 10 years [9,22] after transplantation have provided both qualitative and quantitative measurement of cellular biology outcome of therapeutic fetal grafts. Human fetal grafts in these patients are rather small, representing no more than~4% of the corpus striatum volume and contain less than 60% of P-zones (i.e., region selectively positive for striatal interneurons or for striatal projection neurons markers [22].…”

“…The main challenge for quality control (QC) of fetal grafts is the accuracy of the dissection (in HD clinical trials), either of the whole ganglionic eminences, the LGE, or the far lateral ganglionic eminences, the most lateral half of the LGE. In each cases, the primary focus is on the harvest of tissue that would yield the most DARPP32+ neurons and striatal like tissue (P-zone, i.e., the LGE/far lateral ganglionic eminences) [7,16,22,[74][75][76]. In addition, a secondary focus is on the complementary harvest of tissue to enhance the survival of LGE-derived MSNs or on the restoration of all striatal cell type, as with the harvest of whole GE [6,8,77].…”

“…In the few transplanted patients autopsied, histological analyses at 18 months [21] to 10 years [9,22] after transplantation have provided both qualitative and quantitative measurement of cellular biology outcome of therapeutic fetal grafts. Human fetal grafts in these patients are rather small, representing no more than~4% of the corpus striatum volume and contain less than 60% of P-zones (i.e., region selectively positive for striatal interneurons or for striatal projection neurons markers [22]. These graft-derived Pzones are specifically surrounded by activated microglia, whereas MSNs inside these regions are found more markedly positive for apoptotic markers.…”

Human Pluripotent Stem Cell Therapy for Huntington's Disease: Technical, Immunological, and Safety Challenges

Embryonic or Neural Stem Cells in Neurodegenerative Disease of the Central Nervous System (with Relevance to PD, HD, AD, MS, SCI, and Stroke)