AI Article Synopsis

  • Immunohistochemistry (IHC) is crucial for studying neurochemical molecules in the developing human brain, but existing protocols are inadequate for fragile fetal brains, particularly those fixed using the non-perfusion method.
  • This study improves IHC methods by optimizing antigen retrieval and visualization techniques specific for formalin-fixed fetal brain tissue, demonstrating effective use of antibodies with minimal tissue damage.
  • The new protocol offers a reliable and high-quality approach for studying the fetal brain's chemoarchitecture, addressing past issues related to tissue damage and inferior antigen expression, and is applicable across various gestational ages.

Article Abstract

Background: Immunohistochemistry (IHC) is an important technique in understanding the expression of neurochemical molecules in the developing human brain. Despite its routine application in the research and clinical setup, the IHC protocol specific for soft fragile fetal brains that are fixed using the non-perfusion method is still limited in studying the whole brain.

New Method: This study shows that the IHC protocols, using a chromogenic detection system, used in animals and adult humans are not optimal in the fetal brains. We have optimized key steps from Antigen retrieval (AR) to chromogen visualization for formalin-fixed whole-brain cryosections (20 µm) mounted on glass slides.

Results: We show the results from six validated, commonly used antibodies to study the fetal brain. We achieved optimal antigen retrieval with 0.1 M Boric Acid, pH 9.0 at 70°C for 20 minutes. We also present the optimal incubation duration and temperature for protein blocking and the primary antibody that results in specific antigen labeling with minimal tissue damage.

Comparison With Existing Methods: The IHC protocol commonly used for adult human and animal brains results in significant tissue damage in the fetal brains with little or suboptimal antigen expression. Our new method with important modifications including the temperature, duration, and choice of the alkaline buffer for AR addresses these pitfalls and provides high-quality results.

Conclusion: The optimized IHC protocol for the developing human brain (13-22 GW) provides a high-quality, repeatable, and reliable method for studying chemoarchitecture in neurotypical and pathological conditions across different gestational ages.

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Source
http://dx.doi.org/10.1016/j.jneumeth.2024.110085DOI Listing

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