Mutations within the propeptide, the primary cleavage site or the catalytic site, or deletion of C-terminal sequences, prevents secretion of proPC2 from transfected COS-7 cells

PC2 is a neuroendocrine endoprotease involved in the processing of prohormones and proneuropeptides. PC2 is synthesized as a proenzyme which undergoes proteolytic maturation within the cellular secretory apparatus. Cleavage occurs at specific sites to remove the N-terminal propeptide. The aim of the...

Full description

Saved in:

Bibliographic Details
Published in:	Biochemical journal Vol. 321 ( Pt 2); no. 2; pp. 367 - 373
Main Authors:	Taylor, N A, Shennan, K I, Cutler, D F, Docherty, K
Format:	Journal Article
Language:	English
Published:	England 15-01-1997
Subjects:	Amino Acid Sequence - genetics Animals Binding Sites - genetics Catalysis COS Cells Mutagenesis, Site-Directed Peptide Fragments - genetics Peptide Fragments - physiology Proprotein Convertase 2 Protein Precursors - genetics Protein Precursors - physiology Sequence Deletion Subtilisins - genetics Subtilisins - metabolism Transfection
Online Access:	Get full text
Tags:	Add Tag No Tags, Be the first to tag this record!

Abstract	PC2 is a neuroendocrine endoprotease involved in the processing of prohormones and proneuropeptides. PC2 is synthesized as a proenzyme which undergoes proteolytic maturation within the cellular secretory apparatus. Cleavage occurs at specific sites to remove the N-terminal propeptide. The aim of the present study was to investigate structural requirements for the transfer of proPC2 through the secretory pathway. A series of mutant proPC2 constructs were transfected into COS-7 cells and the fate of the expressed proteins followed by pulse-chase analysis and immunocytochemistry. Human PC2 was secreted relatively slowly, and appeared in the medium primarily as proPC2 (75 kDa), together with much lower amounts of a processed intermediate (71 kDa) and mature PC2 (68 kDa). Mutations within the primary processing site or the catalytic triad caused the protein to accumulate intracellularly, whereas deletion of part of the propeptide, the P-domain or the C-terminal regions also prevented secretion. Immunocytochemistry showed that wild-type hPC2 was localized mainly in the Golgi, whereas two representative mutants showed a distribution typical of proteins resident in the endoplasmic reticulum. The results suggest that proenzyme processing is not essential for secretion of PC2, but peptides containing mutations that affect the ability of the propeptide (and cleavage sites) to fold within the catalytic pocket are not transferred beyond the early stages of the secretory pathway. C-terminal sequences may be involved in stabilizing such conformations.
AbstractList	PC2 is a neuroendocrine endoprotease involved in the processing of prohormones and proneuropeptides. PC2 is synthesized as a proenzyme which undergoes proteolytic maturation within the cellular secretory apparatus. Cleavage occurs at specific sites to remove the N-terminal propeptide. The aim of the present study was to investigate structural requirements for the transfer of proPC2 through the secretory pathway. A series of mutant proPC2 constructs were transfected into COS-7 cells and the fate of the expressed proteins followed by pulse-chase analysis and immunocytochemistry. Human PC2 was secreted relatively slowly, and appeared in the medium primarily as proPC2 (75 kDa), together with much lower amounts of a processed intermediate (71 kDa) and mature PC2 (68 kDa). Mutations within the primary processing site or the catalytic triad caused the protein to accumulate intracellularly, whereas deletion of part of the propeptide, the P-domain or the C-terminal regions also prevented secretion. Immunocytochemistry showed that wild-type hPC2 was localized mainly in the Golgi, whereas two representative mutants showed a distribution typical of proteins resident in the endoplasmic reticulum. The results suggest that proenzyme processing is not essential for secretion of PC2, but peptides containing mutations that affect the ability of the propeptide (and cleavage sites) to fold within the catalytic pocket are not transferred beyond the early stages of the secretory pathway. C-terminal sequences may be involved in stabilizing such conformations. PC2 is a neuroendocrine endoprotease involved in the processing of prohormones and proneuropeptides. PC2 is synthesized as a proenzyme which undergoes proteolytic maturation within the cellular secretory apparatus. Cleavage occurs at specific sites to remove the N-terminal propeptide. The aim of the present study was to investigate structural requirements for the transfer of proPC2 through the secretory pathway. A series of mutant proPC2 constructs were transfected into COS-7 cells and the fate of the expressed proteins followed by pulseŐchase analysis and immunocytochemistry. Human PC2 was secreted relatively slowly, and appeared in the medium primarily as proPC2 (75 kDa), together with much lower amounts of a processed intermediate (71 kDa) and mature PC2 (68 kDa). Mutations within the primary processing site or the catalytic triad caused the protein to accumulate intracellularly, whereas deletion of part of the propeptide, the P-domain or the C-terminal regions also prevented secretion. Immunocytochemistry showed that wild-type hPC2 was localized mainly in the Golgi, whereas two representative mutants showed a distribution typical of proteins resident in the endoplasmic reticulum. The results suggest that proenzyme processing is not essential for secretion of PC2, but peptides containing mutations that affect the ability of the propeptide (and cleavage sites) to fold within the catalytic pocket are not transferred beyond the early stages of the secretory pathway. C-terminal sequences may be involved in stabilizing such conformations.
Author	Cutler, D F Shennan, K I Taylor, N A Docherty, K
AuthorAffiliation	Department of Molecular and Cell Biology, University of Aberdeen, U.K
AuthorAffiliation_xml	– name: Department of Molecular and Cell Biology, University of Aberdeen, U.K
Author_xml	– sequence: 1 givenname: N A surname: Taylor fullname: Taylor, N A organization: Department of Molecular and Cell Biology, University of Aberdeen, U.K – sequence: 2 givenname: K I surname: Shennan fullname: Shennan, K I – sequence: 3 givenname: D F surname: Cutler fullname: Cutler, D F – sequence: 4 givenname: K surname: Docherty fullname: Docherty, K
BackLink	https://www.ncbi.nlm.nih.gov/pubmed/9020868$$D View this record in MEDLINE/PubMed
BookMark	eNpVkd1q3DAQhUVJSTZpL_oAAd0G1ulIsi35phBM_iAlhbbXRpbHWQWvtJW0G_at-ojRJsvSXok5c-YbSeeUHDnvkJAvDC4ZlPxr_yw4A1HLD2TGSgmFklwdkRnwuixq4OyEnMb4DMBKKOGYHDfAQdVqRv5-XyedrHeRvti0sI6mBdJV8CtcJTvgfF_bpQ5baibUG_2ENNqE1Ie3ptFJT9tkzZs638kDTriDUj_StkgYltbpiUb8s0ZnMM4zETfoUsyaCQdv3vuj5XQMfklT0C6OaBIOtH38WUhqcJriJ_Jx1FPEz_vzjPy-uf7V3hUPj7f37dVDYYSEVNS8zE-UvK8USsFE36hKSMVBaFE1ojeNQKk1VBVTA-emVnzAJs-MudLNKM7It3fuat0vcTD5skFP3f4nOq9t93_H2UX35Dcd40yBVBlw8Q4wwccYcDzMMuh2qXWH1LL3_N9lB-c-JvEKE5qXPg
CitedBy_id	crossref_primary_10_1074_jbc_M003547200 crossref_primary_10_3389_fnmol_2015_00045 crossref_primary_10_4199_C00050ED1V01Y201112NPE001 crossref_primary_10_1038_ng0797_303 crossref_primary_10_1371_journal_pone_0108878 crossref_primary_10_1016_j_abb_2004_03_020 crossref_primary_10_1016_j_bbrc_2007_02_034 crossref_primary_10_1080_10409238_2020_1742090 crossref_primary_10_1006_abbi_1998_1033 crossref_primary_10_1515_bmc_2010_025 crossref_primary_10_1074_jbc_274_18_12461 crossref_primary_10_1128_MCB_18_1_400 crossref_primary_10_1074_jbc_M208009200 crossref_primary_10_7554_eLife_19755 crossref_primary_10_1074_jbc_M000032200 crossref_primary_10_1074_jbc_273_47_31574 crossref_primary_10_1210_en_2010_0296 crossref_primary_10_1016_S0014_5793_98_00480_3 crossref_primary_10_1139_w01_144 crossref_primary_10_1007_s10930_008_9143_2
ContentType	Journal Article
DBID	CGR CUY CVF ECM EIF NPM AAYXX CITATION 5PM
DOI	10.1042/bj3210367
DatabaseName	Medline MEDLINE MEDLINE (Ovid) MEDLINE MEDLINE PubMed CrossRef PubMed Central (Full Participant titles)
DatabaseTitle	MEDLINE Medline Complete MEDLINE with Full Text PubMed MEDLINE (Ovid) CrossRef
DatabaseTitleList	MEDLINE CrossRef
Database_xml	– sequence: 1 dbid: ECM name: MEDLINE url: https://search.ebscohost.com/login.aspx?direct=true&db=cmedm&site=ehost-live sourceTypes: Index Database
DeliveryMethod	fulltext_linktorsrc
Discipline	Anatomy & Physiology Chemistry
EISSN	1470-8728
EndPage	373
ExternalDocumentID	10_1042_bj3210367 9020868
Genre	Research Support, Non-U.S. Gov't Journal Article
GroupedDBID	--- -DZ -~X .55 .GJ 0R~ 23N 2WC 3EH 3O- 53G 5GY 5RE 5VS 6J9 79B AABGO AAHRG ABPPZ ABTAH ACGFO ACGFS ACNCT ADBBV AEGXH AENEX AI. AIAGR AIZAD ALMA_UNASSIGNED_HOLDINGS BAWUL CGR CS3 CUY CVF DU5 E3Z EBS ECM EIF EJD F20 F5P H13 HH6 HYE HZ~ K-O L7B MV1 MVM N9A NPM O9- OHT OK1 P2P RHI RNS RPM RPO TR2 TWZ VH1 WH7 WOQ X7M XOL XSW Y6R YNY ZGI ZXP ZY4 ~02 ~KM AAYXX CITATION 5PM
ID	FETCH-LOGICAL-c370t-62402072b58e7313b985378203a3593bc93e7aa05518d22c682de9402fd22a9f3
IEDL.DBID	RPM
ISSN	0264-6021
IngestDate	Tue Sep 17 21:22:09 EDT 2024 Thu Nov 21 21:00:51 EST 2024 Sat Sep 28 08:34:43 EDT 2024
IsDoiOpenAccess	false
IsOpenAccess	true
IsPeerReviewed	true
IsScholarly	true
Issue	2
Language	English
LinkModel	DirectLink
MergedId	FETCHMERGED-LOGICAL-c370t-62402072b58e7313b985378203a3593bc93e7aa05518d22c682de9402fd22a9f3
OpenAccessLink	https://europepmc.org/articles/pmc1218078?pdf=render
PMID	9020868
PageCount	7
ParticipantIDs	pubmedcentral_primary_oai_pubmedcentral_nih_gov_1218078 crossref_primary_10_1042_bj3210367 pubmed_primary_9020868
PublicationCentury	1900
PublicationDate	1997-Jan-15 1997-01-15 19970115
PublicationDateYYYYMMDD	1997-01-15
PublicationDate_xml	– month: 01 year: 1997 text: 1997-Jan-15 day: 15
PublicationDecade	1990
PublicationPlace	England
PublicationPlace_xml	– name: England
PublicationTitle	Biochemical journal
PublicationTitleAlternate	Biochem J
PublicationYear	1997
SSID	ssj0014040
Score	1.6880503
Snippet	PC2 is a neuroendocrine endoprotease involved in the processing of prohormones and proneuropeptides. PC2 is synthesized as a proenzyme which undergoes...
SourceID	pubmedcentral crossref pubmed
SourceType	Open Access Repository Aggregation Database Index Database
StartPage	367
SubjectTerms	Amino Acid Sequence - genetics Animals Binding Sites - genetics Catalysis COS Cells Mutagenesis, Site-Directed Peptide Fragments - genetics Peptide Fragments - physiology Proprotein Convertase 2 Protein Precursors - genetics Protein Precursors - physiology Sequence Deletion Subtilisins - genetics Subtilisins - metabolism Transfection
Title	Mutations within the propeptide, the primary cleavage site or the catalytic site, or deletion of C-terminal sequences, prevents secretion of proPC2 from transfected COS-7 cells
URI	https://www.ncbi.nlm.nih.gov/pubmed/9020868 https://pubmed.ncbi.nlm.nih.gov/PMC1218078
Volume	321 ( Pt 2)
hasFullText	1
inHoldings	1
isFullTextHit
isPrint
link	http://sdu.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1LbxMxEB6RSoheELRUhAIaIcQpbja21949VkurXgqVChK3yF5vRFCzqfJA6r_iJ3bG8a6aK0e_VzuWv3n5M8DnOi-MIRgSwTgnCG8LQXpzIULwTmrj1CzwReGrW_vtV_H1gmly8u4uTEzar_38rL1bnLXz3zG38n5Rj7s8sfHNdTUhXCJoGw9gQLphZ6Kn0IHOdHKsaGEIwTo6IS3H_g_fWFHGHsLzkl-nZILVJ3DUY9B-fuQTwLl8BS-Tpojnuy96Dc-a9giOz1uykhcP-AVj7mZ0ih_Bi6p7t-0Y_l1vd-H1NbKTdd4i6Xh4z053Oh5CM0rlyDKBNLX7S2cKchQZl6vYGH06D7RurB1xNb-Xw5PicoaVSCk0d9hnYo9oxkgGtaa6etX3pXVvKol8iwU3UUmmE7YJWH2_FRY5bLB-Az8vL35UVyK9yyBqZbONMByRyaz0edFYNVG-JMxn3j3lVF4qX5eqsc5lTPYWpKxNIUNT0pgZlVw5Uydw0C7b5i2g9WR_WTLBpPFkqhUul0FL74IOpfY-G8KnTjzT9GOmMWyu5bSX5hBOdvLquyThDsHuCbJvZ07t_RbaapFbO22td_898hQOdwy3EzHJ38PBZrVtPsBgHbYf4z59BELq714
link.rule.ids	230,315,729,782,786,887,27933,27934,53800,53802
linkProvider	National Library of Medicine
linkToHtml	http://sdu.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1bT9swFD4aTBO8DAZD68bY0TTtqaap7djJI8pAnUYZEkzaW2XHqehEU9TLJP7VfuKOXSeirzzGx5coPvG5fwb4UqaZUiSGmFPGMJK3GSO9OWPOWcOlMmLsfKHw4EZf_c6-nXuYnLSphQlJ-6WdnNb309N6chdyKx-mZa_JE-tdD4s-ySUSbb0teEn_a5I0RnoMHshERteKZIpkWAMoJHnP_vE1K0LpXXiV-_spPcTqE4HUSqHNDMknIudi75kvuw-vo46JZ2vyG3hR1QdweFaTfT19xK8Ysj6DO_0AdormxrdD-DdcrQPzC_Tu2UmNpB3ig3fX08Hiqm58DvgUSFObv3QaoY8_42weiMEb9Ejrhtaub_Y37fhJcTbGgsXkm3tsc7i7NGOAkVpQWzlv-9K61wVHX_-Cy6Be09lcOSx-3jCNPuCweAu_Ls5viwGLNzqwUuhkyZSP5SSa2zSrtOgLm5O24BH7hBFpLmyZi0obk3iYOMd5qTLuqpzGjOnJ5GNxBNv1rK7eAWpLlpsm440rS0ZeZlLuJLfGSZdLa5MOfG62dRQ_zCgE3CUftVzQgaP1PrddIlN0QG8wQEv3aNybFNr3gMod9_n9s0d-gp3B7fBydPn96scH2F3j5PZZPz2G7eV8VX2ErYVbnQRe_w_eQgTw
linkToPdf	http://sdu.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwpV1bT9swFD4aTNt4GRsMrTCYNU081U1qO3byiAIVaINVYkh7q-w40TrRtOplEv9qP3HHrhPRV3iMr1HOic_V3wH4WiSplCiGqJVaU5S3KUW9OaXWGs2E1Lyy7qLw5a26-ZWeXziYnLbUl0_aL8y4V99PevX4t8-tnE2KqMkTi4bXeR_lEoq2aGaraAte4j8bs8ZQDwEEEYvgXhFUohxrQIUEi8wfd2-FS7UDrzJXo9LBrD4SSq0k2sySfCR2BrvPeOF38DbomuRsPeQ9vCjrPdg_q9HOnjyQU-KzP71bfQ_e5E3lt334d71aB-gXxLlpxzVBLZHMnNseDxhbdsOzx6kguLT-i6cScXFoMp37Tu8VesB9fWvXNbuKO25RMq1ITkMSzj1pc7m7uKKHk1pgWzFvx-K-w5wRdw-GLL2ajWd0aUn-45Yq4gIPiw9wN7j4mV_SUNmBFlzFSypdTCdWzCRpqXifmwy1BofcxzVPMm6KjJdK69jBxVnGCpkyW2Y4p8InnVX8ALbraV1-BKIMWnAKjTgmDRp7qU6YFcxoK2wmjIk78KUh7Sh8mJEPvAs2ajmhAwdrWrdDAmN0QG0wQdvvULk3e5D2Hp070PrwyTM_w-vh-WD0_erm2xHsrOFy-7SffILt5XxVHsPWwq5OPLv_BwsNB3A
openUrl	ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Mutations+within+the+propeptide%2C+the+primary+cleavage+site+or+the+catalytic+site%2C+or+deletion+of+C-terminal+sequences%2C+prevents+secretion+of+proPC2+from+transfected+COS-7+cells&rft.jtitle=Biochemical+journal&rft.au=Taylor%2C+N+A&rft.au=Shennan%2C+K+I&rft.au=Cutler%2C+D+F&rft.au=Docherty%2C+K&rft.date=1997-01-15&rft.issn=0264-6021&rft.eissn=1470-8728&rft.volume=321&rft.issue=Pt+2&rft.spage=367&rft.epage=373&rft_id=info:doi/10.1042%2Fbj3210367&rft_id=info%3Apmid%2F9020868&rft.externalDBID=PMC1218078
thumbnail_l	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=0264-6021&client=summon
thumbnail_m	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=0264-6021&client=summon
thumbnail_s	http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=0264-6021&client=summon