Purified anti-Neurofilament H (NF-H), Nonphosphorylated Antibody (Previously Covance catalog# SMI-32P)

Pricing & Availability
Clone
SMI 32 (See other available formats)
Regulatory Status
RUO
Other Names
Neurofilament heavy polypeptide, NF-H, 200 kD neurofilament protein, neurofilament triplet H protein
Previously
Covance Catalog# SMI-32P
Isotype
Mouse IgG1
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Product Citations
publications
1_SMI-32_PURE_NF-H_Antibody_IHC-P_011218
IHC staining of purified anti-Neurofilament H (NF-H), Nonphosphorylated antibody (clone SMI 32) on formalin-fixed paraffin-embedded mouse brain tissue. Following antigen retrieval using Retrieval-ALL Antigen Unmasking System 3 (Cat. No. 927601), the tissue was incubated with 1 µg/ml of the primary antibody overnight at 4°C. BioLegend’s Ultra Streptavidin (USA) HRP Detection Kit (Multi-Species, DAB, Cat. No. 929901) was used for detection followed by hematoxylin counterstaining, according to the protocol provided. The image was captured with a 40X objective. Scale bar: 50µm
  • 1_SMI-32_PURE_NF-H_Antibody_IHC-P_011218
    IHC staining of purified anti-Neurofilament H (NF-H), Nonphosphorylated antibody (clone SMI 32) on formalin-fixed paraffin-embedded mouse brain tissue. Following antigen retrieval using Retrieval-ALL Antigen Unmasking System 3 (Cat. No. 927601), the tissue was incubated with 1 µg/ml of the primary antibody overnight at 4°C. BioLegend’s Ultra Streptavidin (USA) HRP Detection Kit (Multi-Species, DAB, Cat. No. 929901) was used for detection followed by hematoxylin counterstaining, according to the protocol provided. The image was captured with a 40X objective. Scale bar: 50µm
  • SMI-32_PURE_NeurofilamentH_Antibody_HR_2_090517
    Immunofluorescence staining of anti-Neurofilament H (NF-H), Nonphosphorylated antibody (clone SMI 32) on formalin-fixed paraffin-embedded (FFPE) tissue section from mouse Thalamus. After antigen retrieval using Retrieval-ALL Antigen Unmasking System 3 (Cat. No. 927601), the tissue was blocked with Normal Serum Block for 30 min at room temperature, and then incubated with SMI 32 at 5 µg/mL overnight at 4°C, followed by incubation with Alexa Fluor® 488 Goat anti-mouse IgG (Cat. No. 405319) for one hour at room temperature. The image was captured with a 40X objective (Scale Bar: 20 µm).
  • SMI-32_PURE_NeurofilamentH_Antibody_HR_3_090517
    IHC-Fluorescence staining of Formalin Fixed Paraffin Embedded (FFPE) Rat Cerebellum by anti-Neurofilament H (NF-H), Nonphosphorylated Antibody clone SMI 32. After antigen retrieval using Retrieval-ALL Antigen Unmasking System 3 (Cat. No. 927601), the tissue was blocked with Normal Serum Block for 30 min at room temperature, and then incubated with SMI 32 at 5 µg/mL overnight at 4°C, followed by incubation with Alexa Fluor® 488 Goat anti-mouse IgG (Cat. No. 405319) for one hour at room temperature. The image was captured with a 40X objective (Scale Bar: 20 µm).
  • SMI-32_PURE_NF-H_Antibody_WB_011218
    Western blot of purified anti-Neurofilament H (NF-H), Nonphosphorylated antibody (clone SMI 32). Lane 1: Molecular weight marker; Lane 2: 20 µg of human brain lysate; Lane 3: 20 µg of mouse brain lysate; Lane 4: 20 µg of rat brain lysate. The blot was incubated with 1 ug/mL of the primary antibody overnight at 4°C, followed by incubation with HRP-labeled goat anti-mouse IgG (Cat. No. 405306). Enhanced chemiluminescence was used as the detection system.
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Description

Neurofilaments (NF) are approximately 10 nanometer intermediate filaments found in neurons. They are a major component of the neuronal cytoskeleton, and function primarily to provide structural support for the axon and to regulate the axon diameter. There are three major NF subunits, and the names given to these subunits are based upon the apparent molecular mass of the mammalian subunits on SDS-PAGE. The light or lowest NF (NF-L) runs at 68-70 kD. The medium or middle NF (NF-M) runs at about 145-160 kD, and the heavy or highest NF (NF-H) runs at 200-220 kD. However, the actual molecular weight of these proteins is considerably lower due to the highly charged C-terminal regions of the molecules. The level of NF gene expression correlates with the axonal diameter, which controls how fast electrical signals travel down the axon. Mutant mice with NF abnormalities have phenotypes resembling amyotrophic lateral sclerosis. NF immunostaining is common in diagnostic neuropathology. It is useful for differentiating neurons (positive for NF) from the glia (negative for NF).

Product Details
Technical data sheet

Product Details

Verified Reactivity
Human, Mouse, Rat
Antibody Type
Monoclonal
Host Species
Mouse
Formulation
Phosphate-buffered solution (no preservatives or carrier proteins).
Preparation
The antibody was purified by affinity chromatography.
Concentration
1 mg/ml
Storage & Handling
This antibody should be handled aseptically as it is free of preservatives such as Sodium Azide. Store this antibody undiluted between 2°C and 8°C. Please note the storage condition for this antibody has been changed from -20°C to between 2°C and 8°C. You can also check the vial label or CoA to find the proper storage conditions.
Application

IHC-P - Quality tested
WB - Verified
Array Tomography, ICC - Reported in the literature, not verified in house
SB - Community verified

Recommended Usage

Each lot of this antibody is quality control tested by formalin-fixed paraffin-embedded immunohistochemical staining. For immunohistochemistry, a concentration range of 1.0 - 5.0 µg/ml is suggested. For Western blotting, the suggested use of this reagent is 1.0 - 5.0 µg per ml. It is recommended that the reagent be titrated for optimal performance for each application.

Application Notes

Additional reported applications (for the relevant formats) include Western blotting6, immunohistochemistry4,5, immunocytochemistry1,2,3, 7, array tomography8.

Cross-reactivity to monkey tissue has been Reported in the literature, not verified in house4.

This antibody reacts with a nonphosphorylated epitope in neurofilament H of most mammalian species. The reaction is masked when the epitope is phosphorylated. The staining of isolated neurofilament preparations is greatly intensified upon dephosphorylation. Immunocytochemically, SMI 32 visualizes neuronal cell bodies, dendrites, and some thick axons in the central and peripheral nervous systems. However, thin axons are not revealed. Other cells and tissues are unreactive. The antibody distinguishes three subdivisions of the macaque precentral motor cortex. The greater size of the left versus the right superior temporal lobe was found to be due to increased axonal myelination and not due to increased number of glial cells or SMI 32-enumerated neurons, suggesting that the specialization for language in the left temporal lobe is related to increased speed of signal transmission. In cultures of murine cortex, SMI 32 labels a neuronal population with enhanced vulnerability to kainate toxicity most of which are GABAergic and reveal kainate-activated Ca2+ uptake.

Additional Product Notes

This product has been verified for IHC-P (Immunohistochemistry - formalin-fixed paraffin-embedded tissues) on the NanoString GeoMx® Digital Spatial Profiler. The GeoMx® enables researchers to perform spatial analysis of protein and RNA targets in FFPE and fresh frozen human and mouse samples. For more information about our spatial biology products and the GeoMx® platform, please visit our spatial biology page.

Application References

(PubMed link indicates BioLegend citation)
  1. Chang Q, Martin LJ. 2011. J. Neurosci., 31:2815-27. (ICC) PubMed
  2. Stevens HE, et al. 2010. J. Neurosci. 30:5590-602. (ICC) PubMed
  3. Kiryu-Seo S, et al. 2010. J. Neurosci. 30:6658-66. (ICC) PubMed  
  4. Redondo J, et al. 2015. Brain Pathol. 25(6):692. (IHC-P) PubMed  
  5. Feng L, et al. 2017. eNeuro. 4(1): 0331-16.2016. (IHC-P) PubMed
  6. Feng L, et al. 2014. Invest Ophthalmol Vis Sci. 54(2): 1106–1117. (IHC-P) PubMed
  7. Theotokis, et al. 2016. J. Neuroinflammation 13(1):265 (IHC-P)
  8. Bennett, et al. 2015. J. Neurosci. Methods 245:25-36 (Array Tomography)
  9. Petzold A, et al. 2011. Brain 134:464. (WB) PubMed  
Product Citations
  1. Castelli LM, et al. 2021. Mol Neurodegener. 16:53. PubMed
  2. Tsolias A, et al. 2022. Front Neural Circuits. 15:795325. PubMed
  3. Munot P, et al. 2021. Neuropathol Appl Neurobiol. Online ahead of print. PubMed
  4. Hodgetts SI, et al. 2022. Neural Regen Res. 17:1376. PubMed
  5. Tan H, et al. 2022. J Comp Neurol. 530:1276. PubMed
  6. Gao J, et al. 2022. J Comp Neurol. 530:1494. PubMed
  7. McDonald AJ, et al. 2022. Brain Res. 1777:147767. PubMed
  8. Southam K, et al. 2022. J Physiol. 600:1611. PubMed
  9. Riechers SP, et al. 2022. Mol Metab. 60:101468. PubMed
  10. Caval-Holme FS, et al. 2022. J Neurosci. 42:4101. PubMed
  11. Kowal TJ, et al. 2022. J Comp Neurol. 530:2176. PubMed
  12. Ballester-Rosado CJ, et al. 2022. Ann Neurol. 92:45. PubMed
  13. Cunningham ME 2022. Experimental Neurology. 355:114127. PubMed
  14. Weil T, et al. 2022. Sci Adv. 8:eabn3567. PubMed
  15. Gaja-Capdevila N, et al. 2022. Int J Mol Sci. 23: . PubMed
  16. Januel C, et al. 2022. Cell Mol Life Sci. 79:441. PubMed
  17. Ma C, et al. 2022. J Leukoc Biol. 112:1387. PubMed
  18. Rosas Almanza J, et al. 2022. J Neurosci Res. 100:2213. PubMed
  19. Kapar O, et al. 2022. Neurosurg Focus. 53:E6. PubMed
  20. Gallego-Ortega A, et al. 2022. Front Neuroanat. 16:1054849. PubMed
  21. Zhang Y, et al. 2022. Front Cell Neurosci. 16:1069617. PubMed
  22. Kumar MS, et al. 2022. Int J Mol Sci. 23: . PubMed
  23. Tsitsipatis D, et al. 2022. Aging (Albany NY). 14:9832. PubMed
  24. Montilla A, et al. 2023. Cell Death Dis. 14:16. PubMed
  25. Li Z, et al. 2023. J Neuroinflammation. 20:16. PubMed
  26. Kapell H, et al. 2023. J Clin Invest. :. PubMed
  27. Zhang S, et al. 2022. Neuron. 110:992. PubMed
  28. Pellegatta M, et al. 2022. J Neurosci. 42:2433. PubMed
  29. Hagemann C, et al. 2022. Adv Healthc Mater. 11:e2101817. PubMed
  30. Zhu PP, et al. 2022. Hum Mol Genet. 31:2779. PubMed
  31. Stevens H, et al. 2010. J Neurosci. 30:5590-5602. PubMed
  32. Cignarella F et al. 2018. Cell metabolism. 27(6):1222-1235 . PubMed
  33. Zhou Y, et al. 2019. J Clin Invest. 130:1756. PubMed
  34. Abernathy DG et al. 2017. Cell stem cell. 21(3):332-348 . PubMed
  35. Zhang LY, et al. 2020. Theranostics. 0.468055556. PubMed
  36. Beckman D, et al. 2022. Cell Rep. 41:111573. PubMed
  37. Metzner K, et al. 2022. Front Cell Dev Biol. 10:965382. PubMed
  38. Matsuda K, et al. 2022. Cereb Cortex Commun. 3:tgac046. PubMed
  39. Pinton L, et al. 2023. Nat Protoc. 18:1337. PubMed
  40. Jia J, et al. 2023. Cell Death Dis. 14:156. PubMed
  41. Castellanos-Montiel MJ, et al. 2023. Cells. 12:. PubMed
  42. Pestronk A, et al. 2023. Neuropathol Appl Neurobiol. 49:e12898. PubMed
  43. Schmitt LI, et al. 2023. Acta Neuropathol. 145:611. PubMed
  44. Zahaf A, et al. 2023. Nat Commun. 14:1592. PubMed
  45. Hazra R, et al. 2023. Biomedicines. 11:. PubMed
  46. Chen TH, et al. 2023. Mol Ther Nucleic Acids. 32:144. PubMed
  47. Fiedler T, et al. 2023. J Neuroinflammation. 20:100. PubMed
  48. Del Bondio A, et al. 2023. JCI Insight. 8:. PubMed
  49. Samtani G, et al. 2023. Front Cell Neurosci. 17:1169786. PubMed
  50. Abdelwahab T, et al. 2023. iScience. 26:106698. PubMed
  51. Ruff T, et al. 2021. Front Mol Neurosci. 14:790466. PubMed
  52. Bakken TE, et al. 2021. Nature. 598:111. PubMed
  53. Rosenkranz SC, et al. 2021. eLife. 10:00. PubMed
  54. Cocozza G, et al. 2018. Brain Behav Immun. 73:584. PubMed
  55. Penndorf D et al. 2017. PloS one. 12(8):e0183684 . PubMed
  56. Atkinson R, et al. 2021. Dis Model Mech. 14:dmm047548. PubMed
  57. Sherafat A, et al. 2021. Nat Commun. 12:2265. PubMed
  58. Manivasagam S, et al. 2022. J Immunol. 208:1341. PubMed
  59. Leo M, et al. 2022. Cells. 11:. PubMed
  60. Li X, et al. 2017. Mol Ther. 25(1):140-152. PubMed
  61. Trikamji B, et al. 2021. Muscle Nerve. 63:506. PubMed
  62. Ding B, et al. 2021. J Neurosci. 41:2024. PubMed
  63. Mahajan KR, et al. 2020. Ann Neurol. 88:81. PubMed
  64. Mikhalkin A, et al. 2020. Journal of Comparative Neurology. 529(7):1430-1441. PubMed
  65. Yoo M, Kim T 2016. Sci Rep. 6:28548. PubMed
  66. Gaja-Capdevila N, et al. 2021. Front Pharmacol. 12:780588. PubMed
  67. Sainio MT, et al. 2022. Front Cell Dev Biol. 9:820105. PubMed
  68. Shi L, et al. 2021. Immunity. . PubMed
  69. Corsini S, et al. 2017. Cell Death Dis. 10.1038/cddis.2017.232. PubMed
  70. Wong R, et al. 2019. Brain Behav Immun. 76:126. PubMed
  71. Zhang Q, et al. 2019. PLoS Biol. 17:e3000330. PubMed
  72. Drohomyrecky PC, et al. 2019. J Immunol. 203:2588. PubMed
  73. Doust YV, et al. 2021. Front Neurol. 12:722526. PubMed
  74. Utagawa EC, et al. 2022. Acta Neuropathol Commun. 10:86. PubMed
  75. Shi X, et al. 2021. Nat Commun. 12:6943. PubMed
  76. Prukop T, et al. 2020. J Neurosci Res. 1933:98. PubMed
  77. Brodie-Kommit J, et al. 2021. Science Advances. 7(11):. PubMed
  78. Saba L, et al. 2016. Cereb Cortex. 26: 1512-1528. PubMed
  79. Li S, et al. 2016. Proc Natl Acad Sci U S A. 113: 1937 - 1942. PubMed
  80. Iida M, et al. 2019. Nat Commun. 10:4262. PubMed
  81. Honig MG, et al. 2021. Front Neurosci. 15:701317. PubMed
  82. , et al. 2021. Nature. 598:151. PubMed
  83. Kondo T, et al. 2022. Front Cell Neurosci. 16:858562. PubMed
  84. Harley J, et al. 2021. Brain Commun. 3:fcab166. PubMed
  85. Calvo-Barreiro L, et al. 2021. Neurotherapeutics. . PubMed
  86. Merkulyeva N, et al. 2021. Neuroscience Letters. 762:136165. PubMed
  87. Reinhard K, et al. 2020. eLife. 8:e50697.. PubMed
  88. Ondatje BN, et al. 2022. Lab Chip. 22:4246. PubMed
  89. Sharf T, et al. 2022. Nat Commun. 13:4403. PubMed
  90. Mavlyutov TA, et al. 2022. Cell Biosci. 12:72. PubMed
  91. Chen D, et al. 2022. J Neuroinflammation. 19:112. PubMed
  92. Clark CM, et al. 2021. Brain Sci. 11:. PubMed
  93. Simone R, et al. 2021. Nature. 594:117. PubMed
  94. Candadai AA, et al. 2021. PLoS One. e0247901:16. PubMed
  95. Ho R, et al. 2020. Cell Systems. 12(2):159-175.e9. PubMed
  96. Rizzo F, et al. 2016. Hum Mol Genet. 10.1093/hmg/ddw258. PubMed
  97. örner S, et al. 2016. J Neuropathol Exp Neurol. 10.1093/jnen/nlw003. PubMed
  98. Laug D, et al. 2019. J Clin Invest. 129:4408. PubMed
  99. Takakura K, et al. 2017. Heliyon. 3:e00462. PubMed
  100. Tung YT et al. 2019. Cell Stem Cell. 25(2):193-209 . PubMed
  101. Risner ML, et al. 2022. Mol Neurobiol. 59:1366. PubMed
  102. Yu M, et al. 2022. Front Neurol. 13:903565. PubMed
  103. Ou Y, et al. 2016. J Neurosci. 36: 9240 - 9252. PubMed
  104. Himmelein S, et al. 2017. J Virol. 10.1128/JVI.00331-17. PubMed
  105. Miguel JC, et al. 2021. Front Aging Neurosci. 645334:13. PubMed
  106. Yi‐Lan Weng et al. 2018. Neuron. 97(2):313-325 . PubMed
  107. McLeod VM et al. 2019. Br J Pharmacol. 176(13):2111-2130 . PubMed
  108. Schirmer L, et al. 2019. Nature. 573:75. PubMed
  109. Yang C, et al. 2020. Neuron. 105:276. PubMed
  110. Abo-Rady M, et al. 2020. Stem Cell Reports. 14:390. PubMed
  111. Ben Haim L, et al. 2021. Glia. 69:2812. PubMed
  112. van der Heijden ME, et al. 2021. J Physiol. 599:2037. PubMed
  113. Jiang D, et al. 2019. Journal of Comparative Neurology. 528(5):729-755. PubMed
  114. Azeez I, et al. 2016. J Neuropathol Exp Neurol. 75: 843 - 854. PubMed
  115. Donkels C, et al. 2016. Cereb Cortex. 10.1093/cercor/bhv346. PubMed
  116. Saraf MP et al. 2019. The Journal of comparative neurology. 527(15):2599-2611 . PubMed
  117. Groh J, et al. 2021. Brain Commun. 3:fcab047. PubMed
  118. Petrozziello T, et al. 2017. Cell Death Differ. 10.1038/cdd.2016.154. PubMed
  119. Chavali M, et al. 2020. Neuron. . PubMed
  120. Kinoshita H, et al. 2019. Sci Rep. 9:11519. PubMed
  121. Okigawa S, et al. 2021. J Comp Neurol. 529:2099. PubMed
  122. Lanz T, et al. 2017. Sci Rep. 7:41271. PubMed
  123. Brambilla L, et al. 2016. Hum Mol Genet. 10.1093/hmg/ddw161. PubMed
  124. Ebert T 2016. Hum Mol Genet. 25: 514 - 523. PubMed
  125. Roboon J, et al. 2019. Front Cell Neurosci. 13:258. PubMed
  126. van der Heijden ME, et al. 2021. Elife. 10:. PubMed
  127. Wolf C, et al. 2022. Commun Biol. 5:541. PubMed
  128. Parisi C, et al. 2016. Cell Death Differ. 23:531-541. PubMed
  129. Wagener R, et al. 2016. Cereb Cortex. 26: 820 - 837. PubMed
  130. Ho R, et al. 2016. Nat Neurosci. 10.1038/nn.4345. PubMed
  131. Hughes RO, et al. 2021. Cell Reports. 34(1):108588. PubMed
  132. Ito K, et al. 2018. Sci Rep. 33:1052. PubMed
  133. Saraf MP et al. 2018. The Journal of comparative neurology. 527(3):625-639 . PubMed
  134. Hirono M, et al. 2018. J Neurosci. 38:6130. PubMed
  135. Reinehr S, et al. 2019. Int J Mol Sci. 2.613194444. PubMed
  136. Tan H, et al. 2019. Cell Death Differ. 27:1369. PubMed
  137. Puller C, et al. 2020. J Neurosci. 40:1302. PubMed
  138. Casanovas A, et al. 2017. Sci Rep. 7:40155. PubMed
  139. Berry R, et al. 2015. PLoS One. 10: 0144341. PubMed
  140. Wang H, et al. 2015. Sci Rep. 5: 17383. PubMed
  141. Korzhevskii DE, et al. 2017. Zh Nevrol Psikhiatr Im S S Korsakova. 117:50. PubMed
  142. Dyer M, et al. 2019. Front Aging Neurosci. 11:68. PubMed
  143. Larson VA et al. 2018. eLife. 7 pii: e34829. PubMed
  144. Kelley KW et al. 2018. Neuron. 98(2):306-319 . PubMed
  145. Nelke A, et al. 2022. Front Pharmacol. 12:773925. PubMed
  146. Thiry L, et al. 2022. ASN Neuro. 14:17590914211073381. PubMed
  147. Whye D, et al. 2022. Curr Protoc. 2:e568. PubMed
  148. Martin Q 2011. J Neurosci. 31:2815-2827. PubMed
  149. Petzold A, et al. 2011. Brain. 134:464-483. PubMed
  150. Redondo J, et al. 2015. Brain Pathol. 25:692-700. PubMed
  151. Faustino Martins JM, et al. 2020. Cell Stem Cell. 172:26. PubMed
  152. Miao W, et al. 2020. J Immunol. 1486:204. PubMed
  153. Fouda AY, et al. 2020. Invest Ophthalmol Vis Sci. 51:61. PubMed
  154. De Pace R, et al. 2018. PLoS Genet. 8:6458. PubMed
  155. Jiang LL, et al. 2019. J Clin Invest. 130. PubMed
  156. Pelisch N, et al. 2021. Eneuro. 8:. PubMed
  157. Swanson OK, et al. 2021. Eneuro. 8:. PubMed
  158. Cuadrado E et al. 2019. Cell reports. 26(7):1718-1726 . PubMed
  159. Maruyama T, et al. 2018. Cell Death Dis. 12:146. PubMed
  160. Alcover-Sanchez B, et al. 2021. Glia. 69:619. PubMed
  161. Alpár A, et al. 2018. EMBO J. 37:. PubMed
  162. Wang F, et al. 2021. Current Biology. 31(11):2263-2273.e3. PubMed
  163. Bukreeva I, et al. 2017. Sci Rep. 7:41054. PubMed
  164. Feng L, et al. 2017. eNeuro. 4(1). PubMed
  165. MacNair L, et al. 2016. Brain. 139: 86 - 100. PubMed
  166. Sen T, et al. 2020. J Neurosci. 40:424. PubMed
  167. Litvina EY et al. 2017. Neuron. 96(2):330-338 . PubMed
  168. Abbas Farishta R, et al. 2021. Cereb Cortex Commun. 1:tgaa030. PubMed
  169. Turner M, et al. 2015. J Neuroimmunol. 285: 4-12. PubMed
  170. Pagliarini V, et al. 2015. J Cell Biol. 211: 77 - 90. PubMed
  171. Kiryu-Seo S, et al. 2010. J Neurosci. 30:6658-6666. PubMed
  172. Luna G, et al. 2016. Exp Eye Res. 150: 4-21. PubMed
  173. Roboon J, et al. 2021. Journal of Neurochemistry. . PubMed
  174. Eixarch H, et al. 2020. Neurotherapeutics. 17:1988. PubMed
  175. Wood KC et al. 2017. PloS one. 12(1):e0170264 . PubMed
  176. Granatiero V, et al. 2021. Autophagy. 17:4029. PubMed
  177. Ryan BJ, et al. 2021. J Neurosci. 41:3731. PubMed
  178. Khandker L, et al. 2022. Cell Rep. 38:110423. PubMed
  179. Niu F, et al. 2022. Elife. 11:. PubMed
  180. Henschke JU, et al. 2021. Cell Calcium. 96:102390. PubMed
  181. Richard P, et al. 2020. Autophagy. :1. PubMed
  182. Doroshenko ER, et al. 2021. Front Immunol. 570425:12. PubMed
  183. Wegscheid ML, et al. 2021. Cell Reports. 36(1):109315. PubMed
  184. Salapa HE, et al. 2019. Journal of Neuroscience Research. 98:704. PubMed
  185. Sepehrimanesh M, et al. 2020. American Journal of Physiology-Cell Physiology. 319(4):C771-C780. PubMed
  186. Lv Q, et al. 2021. Cereb Cortex. 31:341. PubMed
  187. Griggs WS et al. 2017. Frontiers in neuroanatomy. 0.531944444 . PubMed
  188. Krieger B, et al. 2017. PLoS One. 12:e0180091. PubMed
RRID
AB_2715852 (BioLegend Cat. No. 801702)
AB_2715852 (BioLegend Cat. No. 801701)

Antigen Details

Structure
Neurofilament H has an apparent molecular mass of 200-220 kD.
Distribution

Tissue distribution: CNS, peripheral nerves and glandular cells of the prostate
Cellular distribution: Cytoskeleton, nucleus, cytosol, and mitochondrion

Function
NF-H Neurofilaments are the major components of the neuronal cytoskeleton. They provide axonal support and regulate axon diameter. Phosphorylation of NF-H results in the formation of interfilament cross bridges that are important in the maintenance of axonal caliber.
Receptors
Phosphorylation seems to play a major role in the functioning of the larger neurofilament polypeptides (NF-M and NF-H), the levels of phosphorylation result in changes to the neurofilament function.
Cell Type
Mature Neurons
Biology Area
Cell Biology, Neuroscience, Neuroscience Cell Markers
Molecular Family
Intermediate Filaments, Phospho-Proteins
Antigen References
  1. Turner M, et al. 2015. Journal of Neuroimmunology. 285: 4. PubMed
  2. Pagliarini V, et al. 2015. J. Cell Biol.. 211: 77. PubMed
  3. Petzold A, et al. 2011. Brain 134. (WB) PubMed 
  4. Yuan A, et al. 2016. Brain Res Bull  126(3): 334.
  5. Parlakian A, et al. 2016. Rev Neurol. 172(10): 607.
  6. Li D, et al. 2016. Front Aging Neurosci. 8: 290.
  7. Costa J, et al. 2016. Clin Chim Acta. 455: 7.
  8. Lad SP, et al. 2010.  J Stroke Cerebrovasc Dis. 21(1): 30.
Gene ID
4744 View all products for this Gene ID
UniProt
View information about Neurofilament H on UniProt.org

Related FAQs

If an antibody clone has been previously successfully used in IBEX in one fluorescent format, will other antibody formats work as well?

It’s likely that other fluorophore conjugates to the same antibody clone will also be compatible with IBEX using the same sample fixation procedure. Ultimately a directly conjugated antibody’s utility in fluorescent imaging and IBEX may be specific to the sample and microscope being used in the experiment. Some antibody clone conjugates may perform better than others due to performance differences in non-specific binding, fluorophore brightness, and other biochemical properties unique to that conjugate.

Will antibodies my lab is already using for fluorescent or chromogenic IHC work in IBEX?

Fundamentally, IBEX as a technique that works much in the same way as single antibody panels or single marker IF/IHC. If you’re already successfully using an antibody clone on a sample of interest, it is likely that clone will have utility in IBEX. It is expected some optimization and testing of different antibody fluorophore conjugates will be required to find a suitable format; however, legacy microscopy techniques like chromogenic IHC on fixed or frozen tissue is an excellent place to start looking for useful antibodies.

Are other fluorophores compatible with IBEX?

Over 18 fluorescent formats have been screened for use in IBEX, however, it is likely that other fluorophores are able to be rapidly bleached in IBEX. If a fluorophore format is already suitable for your imaging platform it can be tested for compatibility in IBEX.

The same antibody works in one tissue type but not another. What is happening?

Differences in tissue properties may impact both the ability of an antibody to bind its target specifically and impact the ability of a specific fluorophore conjugate to overcome the background fluorescent signal in a given tissue. Secondary stains, as well as testing multiple fluorescent conjugates of the same clone, may help to troubleshoot challenging targets or tissues. Using a reference control tissue may also give confidence in the specificity of your staining.

How can I be sure the staining I’m seeing in my tissue is real?

In general, best practices for validating an antibody in traditional chromogenic or fluorescent IHC are applicable to IBEX. Please reference the Nature Methods review on antibody based multiplexed imaging for resources on validating antibodies for IBEX.

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This data display is provided for general comparisons between formats.
Your actual data may vary due to variations in samples, target cells, instruments and their settings, staining conditions, and other factors.
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