2021
DOI: 10.1091/mbc.e20-06-0409
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RTN4B interacting protein FAM134C promotes ER membrane curvature and has a functional role in autophagy

Abstract: The endoplasmic reticulum (ER) is comprised of a controlled ratio of sheets and tubules, which are maintained by several proteins with multiple functions. Reticulons (RTNs), especially RTN4, and DP1/Yop1p family members are known to induce ER membrane curvature. RTN4B is the main RTN4 isoform expressed in non-neuronal cells. In this study, we identified FAM134C as a RTN4B interacting protein in mammalian, non-neuronal cells. FAM134C localized specifically to the ER tubules and sheet edges. Ultrastructural anal… Show more

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Cited by 15 publications
(14 citation statements)
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References 56 publications
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“…Nutrient starvation substantially enhances FAM134B-driven macro-ER-phagy ( 200 ). More recently, FAM134A and FAM134C have also been involved in starvation-induced macro-ER-phagy ( 199 , 206 ). This has led the HUGO gene nomenclature committee to introduce the names Reticulophagy Regulator1 (RETREG1), RETREG2, and RETREG3 for FAM134B, FAM134A, and FAM134C, respectively.…”
Section: Autophagy Of the Er: Er-phagymentioning
confidence: 99%
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“…Nutrient starvation substantially enhances FAM134B-driven macro-ER-phagy ( 200 ). More recently, FAM134A and FAM134C have also been involved in starvation-induced macro-ER-phagy ( 199 , 206 ). This has led the HUGO gene nomenclature committee to introduce the names Reticulophagy Regulator1 (RETREG1), RETREG2, and RETREG3 for FAM134B, FAM134A, and FAM134C, respectively.…”
Section: Autophagy Of the Er: Er-phagymentioning
confidence: 99%
“…The FAM134 proteins contain a reticulon-homology domain at amino acid residues 80–271 (FAM134B), 66–261 (FAM134A), and 53–244 (FAM134C), which is composed of two hydrophobic domains connected by a hydrophilic loop ( FIGURE 8 ). Each hydrophobic domain forms a hairpin within the membrane bilayer without spanning it, promoting high membrane curvature and resulting in both the NH 2 and COOH termini being exposed at the cytosolic leaflet of the ER membrane ( 200 , 206 , 210 , 211 ). The reticulon-homology domain may contribute to membrane deformation, and clustering of FAM134 proteins may facilitate ER fragmentation ( 212 ).…”
Section: Autophagy Of the Er: Er-phagymentioning
confidence: 99%
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“…The term ER-phagy was first coined in 2006 ( Bernales et al., 2006 ) to describe selective degradation of the ER through autophagy, but we started gaining a deeper understanding into the process with the discovery of ER-phagy receptors—mammalian FAM134A, B, and C ( Khaminets et al., 2015 ; Kumar et al., 2021 ; Reggio et al., 2021 ), Sec62 ( Fumagalli et al., 2016 ), RTN3 ( Grumati et al., 2017 ), CCPG1 ( Smith et al., 2018 ), ATL3 ( Chen et al., 2019 ), TEX264 ( An et al., 2019 ; Chino et al., 2019 ), CALCOCO1 ( Nthiga et al., 2020 ), and C53 ( Stephani et al., 2020 ); yeast Atg39, Atg40 ( Mochida et al., 2015 ), and Epr1 ( Zhao et al., 2020 ); and plant ATI1, ATI2, and ATI3 ( Honig et al., 2012 ; Michaeli et al., 2014 ; Zhou et al., 2018 ), Rtn1 and Rtn2 ( Zhang et al., 2020 ), Sec62 ( Hu et al., 2020 ), and C53 ( Stephani et al., 2020 ). All hitherto identified ER-phagy receptors contain an ATG8-interacting motif (AIM), or LIR in mammals, and are localized to the ER.…”
Section: Er-phagymentioning
confidence: 99%
“…FAM134C may be involved in ER-phagy under amino acid starvation. It may also use its LIR to recruit autophagy machinery, and use its RHD to promote the bending and fragmentation of ER [ 41 ]. But the involvement of FAM134A in ER-phagy has not been reported yet.…”
Section: Key Molecules Of Er-phagy (Receptors Cofactors Etc)mentioning
confidence: 99%