Difference between revisions of "Help:Assembly standard 25"

Latest revision as of 20:44, 16 May 2016

The following is adapted from the [http://2007.igem.org/Freiburg07/report_fusion_parts 2007 Albert-Ludwigs Universitat Freiburg iGEM team wiki].

RFC

[http://hdl.handle.net/1721.1/45140 BBF RFC 25: Fusion Protein (Freiburg) Biobrick assembly standard] by Kristian M. Müller, Katja M. Arndt, the 2007 Freiburg iGEM team, and Raik Grünberg

Find RFC25 parts in the RFC25 BioBricks collection.

Background

The generalized BioBrick prefix and suffix with its easy cloning strategy is an excellent and universal way to combine various parts, e.g. promoter region, gene of interest, terminator etc. However, it is not well-suited for in-frame assembly of protein domains due to the 8 bp SpeI/XbaI scar.

Suffix of the first part (part in gray, PstI, NotI, SpeI):

...ACtactagtagcggccgctgcag

combined with Prefix of the second part (EcoRI, NotI, XbaI,part in gray):

gaattccgcggccgcttctagagCA...

results after an SpeI/Xba combination in:

...ACtactagagCA...

encoding the amino acids Tyr (codon: tac), STOP (codon: tag) and Ser or Arg (codon agn).

Consequently, protein domains cannot be designed as separate BioBrick parts and assembled together. The Freiburg assembly standard was developed to address this shortcoming while retaining compatibility with the original BioBrick version. The Freiburg standard extends the original BioBrick standard with two additional compatible restriction sites to allow for the modular assembly of protein fusion parts. For the Freiburg standard, appropriate enzymes were chosen carefully to include ensure coding for amino acids which are compatible with flexible linkers as well as with the N-end rule for protein stability.

Specification

The Freiburg assembly standard extends the original BioBrick suffix and prefix with two additional compatible restriction sites. The frame of the standard suffix and prefix remains the same resulting in complete compatibility with any previously designed parts. We chose the restriction sites NgoMIV and AgeI as they code for the amino acids Ala-Gly or Thr-Gly, respectively, which are compatible with flexible linkers commonly used in fusion proteins and also compatible with the N-end rule for protein stabiliy. Consequently, we name these parts FusionParts. Assembly of two parts that adhere to the Freiburg assembly standard creates an AgeI/NgoMIV scar coding for Thr-Gly, which can easily be integrated in any linker sequence. Furthermore, the NgoMIV site (coding for Ala-Gly) after the start Methionine of the standard BioBrick suffix adheres completely to the N-end rule. For proteins, which are sensitive to amino acid addition at the N-terminus, we also devised an N-Part with a suffix that lacks the NgoMIV site.

The following list summarizes the most important aspects of the Freiburg assembly standard.

Both parts, the FusionPart and the N-part are fully compatible with all standard iGEM parts as they have the BioBricks prefix for coding sequences and the standard BioBrick suffix.
Both parts have two additional enzymes, NgoMIV and AgeI, which have compatible cohesive ends and enable in-frame fusion of protein parts with the linker sequence TG (no stop codons).
The only difference of the N-part and FusionPart is the additional NgoMIV site in the FusionPart.
The FusionPart is the universal part for fusion proteins, and it can be a stand-alone protein part as it has a start codon after the XbaI site (BioBrick prefix for coding sequence), with two additional amino acids (A, G) encoded before the start of the protein.
The N-part is designed to be the start of a fusion protein or a stand-alone protein part, in which the N-terminus is sensitive to any amino acid addition, to be cloned via XbaI/PstI to any iGEM RBS expression part.
The FusionPart can be fused to the N-part by digesting the N-part with AgeI/SpeI and the FusionPart with NgoMIV/SpeI.
Any number of FusionParts can be combined and optionally fused to the N-part.
nnnnnn is a place holder for the coding sequence of the respective part.

Prefix

Freiburg standard FusionPrefix (EcoRI, NotI, XbaI, NgoMIV, part in gray; original BioBrick prefix for coding sequences underlined):

gaattccgcggccgcttctagatggccggcCA...

Freiburg standard N-partPrefix is identical to the BioBrick prefix for coding sequences (EcoRI, NotI, XbaI, part in gray):

gaattccgcggccgcttctagATG...

Suffix

BioBrick 3.0 FusionSuffix (part in gray, AgeI, SpeI, NotI, PstI; original BioBrick suffix underlined):

...ACaccggttaatactagtagcggccgctgcag</b>

Combining the respective prefix and suffix generates the following FusionPart and N-part:

FusionPart

                          NaeI     BsrFI                    SfcI
ApoI                  BsrFI |     BsaWI                 MspA1I|
EcoRI   NotI    XbaI NgoMIV |      AgeI      SpeI    NotI    ||PstI
    |      |       |       | |         |         |       |    ||   |
    GAATTCgcggccgctTCTAGAtgGCCGGCnnnnnnACCGGTtaatACTAGTagcggccgCTGCAG
1 ---------+---------+---------+---------+---------+---------+----- 65
    CTTAAGcgccggcgaAGATCTacCGGCCGnnnnnnTGGCCAattaTGATCAtcgccggcGACGTC
c     I R G R F * M A G  ?  ? T G * Y * * R P L Q   -

N-part

                             BsrFI                    SfcI
ApoI                        BsaWI                 MspA1I|
EcoRI   NotI    XbaI          AgeI      SpeI    NotI    ||PstI
    |      |       |             |         |       |    ||   |
    GAATTCgcggccgctTCTAGAtgnnnnnnACCGGTtaatACTAGTagcggccgCTGCAG
1 ---------+---------+---------+---------+---------+--------- 59
    CTTAAGcgccggcgaAGATCTacnnnnnnTGGCCAattaTGATCAtcgccggcGACGTC
c     I R G R F * M ?  ? T G * Y * * R P L Q   -

Protocols

See [http://openwetware.org/wiki/PrbbBB:Protocols Protocols for assembly of Freiburg parts] on OpenWetWare

References

[http://hdl.handle.net/1721.1/45140 BBF RFC 25: Fusion Protein (Freiburg) Biobrick assembly standard] by Kristian M. Müller, Katja M. Arndt, the 2007 Freiburg iGEM team, and Raik Grünberg

Nishikubo pmid=16140408
Pfleger pmid=16247774
Varshavsky pmid=8901547

</biblio>

[http://www.neb.com/nebecomm/products_Intl/productR0564.asp NgoMIV at NEB]

@@ Line 1: / Line 1: @@
-==Introduction==
+[[Assembly standard 25|< Back to Assembly standard 25 parts]]
+''The following is adapted from the [http://2007.igem.org/Freiburg07/report_fusion_parts 2007 Albert-Ludwigs Universitat Freiburg iGEM team wiki].''
+==RFC==
+*[http://hdl.handle.net/1721.1/45140 BBF RFC 25: Fusion Protein (Freiburg) Biobrick assembly standard] by Kristian M. Müller, Katja M. Arndt, the 2007 Freiburg iGEM team, and Raik Grünberg
+'''Find''' RFC25 parts in the <span style="background:#32CD32">'''[[RFC25_"Freiburg_standard"_parts|RFC25 BioBricks collection]]'''</span>.
+==Background==
 The generalized BioBrick prefix and suffix with its easy cloning strategy is an excellent and universal way to combine  various parts, e.g. promoter region, gene of interest, terminator etc. However, it is not well-suited for in-frame assembly of protein domains due to the 8 bp SpeI/XbaI scar.
@@ Line 16: / Line 25: @@
 <b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;"><font color="#bababa">...AC</font>t<font color="#ff5333">act</font></span><span style="font-family: monospace; font-size: 125%; "><font color="#ff5333">aga</font>g<font color="#bababa">CA...</font></span></b>
-encoding the amino acids Tyr (codon: <codon>tac</codon>), STOP (codon: <code>tag</code>) and Ser or Arg (codon <code>agn</code>).
+encoding the amino acids Tyr (codon: <code>tac</code>), STOP (codon: <code>tag</code>) and Ser or Arg (codon <code>agn</code>).
 Consequently, protein domains cannot be designed as separate BioBrick parts and assembled together.  The Freiburg assembly standard was developed to address this shortcoming while retaining compatibility with the original BioBrick version.  The Freiburg standard extends the original BioBrick standard with two additional compatible restriction sites to allow for the modular assembly of protein fusion parts.  For the Freiburg standard, appropriate enzymes were chosen carefully to include ensure coding for amino acids which are compatible with flexible linkers as well as with the N-end rule  for protein stability.
-==Proposal==
+==Specification==
-The Freiburg assembly standard extends the original BioBrick suffix and prefix with two additional compatible restriction sites. The frame of the standard suffix and prefix remains the same resulting in complete compatibility with any previously designed parts.  We chose the restriction sites NgoMVI and AgeI as they code for
+The Freiburg assembly standard extends the original BioBrick suffix and prefix with two additional compatible restriction sites. The frame of the standard suffix and prefix remains the same resulting in complete compatibility with any previously designed parts.  We chose the restriction sites NgoMIV and AgeI as they code for
-the amino acids Ala-Gly or Thr-Gly, respectively, which are compatible with flexible linkers commonly used in fusion proteins and also compatible with the N-end rule for protein stabiliy.  Assembly of two parts that adhere to the Freiburg assembly standard creates an AgeI/NgoMIV scar coding for Thr-Gly, which can easily be integrated in any linker sequence.  Furthermore, the NgoMIV site (coding for Ala-Gly) after the start Methionine of the standard BioBrick suffix adheres completely to the N-end
+the amino acids Ala-Gly or Thr-Gly, respectively, which are compatible with flexible linkers commonly used in fusion proteins and also compatible with the N-end rule for protein stabiliy.  Consequently, we name these parts '''FusionParts'''.  Assembly of two parts that adhere to the Freiburg assembly standard creates an AgeI/NgoMIV scar coding for Thr-Gly, which can easily be integrated in any linker sequence.  Furthermore, the NgoMIV site (coding for Ala-Gly) after the start Methionine of the standard BioBrick suffix adheres completely to the N-end rule.  For proteins, which are sensitive to amino acid addition at the N-terminus, we also devised an '''N-Part''' with a suffix that lacks the NgoMIV site.
-rule.  For proteins, which are sensitive to amino acid addition at the N-terminus, we also devised an <b>N-Part</b> with a suffix that lacks the NgoMIV site.
 The following list summarizes the most important aspects of the Freiburg assembly standard.
-<p><b><font size="4">Strategy for iGEM BioBrick 3.0 parts for mix-and-match
+*Both parts, the FusionPart and the N-part are fully compatible with all standard iGEM parts as they have the BioBricks prefix for coding sequences and the standard BioBrick suffix.
-construction of fusion proteins  </font></b></p>
+*Both parts have two additional enzymes, NgoMIV and AgeI, which have compatible cohesive ends and enable in-frame fusion of protein parts with the linker sequence TG (no stop codons).
-<p><i>developed by the iGEM Team Freiburg </i>
+*The only difference of the N-part and FusionPart is the additional NgoMIV site in the FusionPart.
-</p>
+*The FusionPart is the universal part for fusion proteins, and it can be a stand-alone protein part as it has a start codon after the XbaI site (BioBrick prefix for coding sequence), with two additional amino acids (A, G) encoded before the start of the protein.
-<ul>
+*The N-part is designed to be the start of a fusion protein or a stand-alone protein part, in which the N-terminus is sensitive to any amino acid addition, to be cloned via XbaI/PstI to any iGEM RBS expression part.
-	<li>Both parts, the FusionPart and the N-part are fully compatible with all standard iGEM parts as they have the
+*The FusionPart can be fused to the N-part by digesting the N-part with AgeI/SpeI and the FusionPart with NgoMIV/SpeI.
-	BioBricks prefix for coding sequences and the standard BioBrick suffix. </li>
+*Any number of FusionParts can be combined and optionally fused to the N-part.
-	<li>Both parts have two additional enzymes, NgoMIV and AgeI, which have
+*nnnnnn is a place holder for the coding sequence of the respective part.
-	compatible cohesive ends and enable in-frame fusion of protein parts with
-	the linker sequence TG (no stop codons). </li>
-	<li>The only difference of the N-part and FusionPart is the additional
-	NgoMIV site in the FusionPart. </li>
-	<li>The FusionPart is the universal part for fusion proteins, and it can be a stand-alone
-	protein part as it has a start codon
-	after the XbaI site (BioBrick prefix for coding sequence), with two
-	additional amino acids (A, G) encoded before the start of the protein.</li>
-	<li>The N-part is designed to be the start of a fusion protein or a
-	stand-alone protein part,, in which the N-terminus is sensitive to any amino
-	acid addition,&nbsp; to be cloned via XbaI/PstI to any iGEM RBS
-	expression part. </li>
-	<li>The FusionPart can be fused to the N-part by digesting the
-	N-part with AgeI/SpeI and the FusionPart with NgoMIV/SpeI. </li>
-	<li>Any number of FusionParts can be combined and optionally fused to the N-part. </li>
-	<li>nnnnnn is a place holder for the coding sequence of the respective part.
-	</li>
-</ul>
+===Prefix===
+Freiburg standard FusionPrefix (<font color="#cc00ff">EcoRI</font>, NotI,<font color="#ff5333"> XbaI</font>,<font color="#bababa"> </font><font color="#009999">NgoMIV</font>,<font color="#bababa"> part in gray</font>; original BioBrick prefix for coding sequences underlined):
-<p><b>Prefix</b></p>
+<b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;"><u><font color="#cc00ff">gaattcc</font>gcggccgct</u><font color="#ff5333"><u>tctag</u>a</font>tg<font color="#009999">gccggc</font><font color="#bababa">CA...</font></span></b>
-<div style="border-style: solid; border-width: 1px; padding-left: 4px; padding-right: 4px; padding-top: 1px; padding-bottom: 1px">
-	BioBrick 3.0 FusionPrefix (<font color="#cc00ff">EcoRI</font>, NotI,<font color="#ff5333">
+Freiburg standard N-partPrefix is identical to the BioBrick prefix for coding sequences (<font color="#cc00ff">EcoRI</font>, NotI,<font color="#ff5333"> XbaI</font>,<font color="#bababa"> part in gray)</font>:
-XbaI</font>,<font color="#bababa"> </font><font color="#009999">NgoMIV</font>,<font color="#bababa"> part in gray</font>;
-	original BioBrick prefix for coding sequences underlined):<p><b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;">
+<b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;"><font color="#cc00ff">gaattcc</font>gcggccgct<font color="#ff5333">tctag</font><font color="#bababa">ATG...</font></span></b>
-	<u>
-<font color="#cc00ff">gaattcc</font>gcggccgct</u><font color="#ff5333"><u>tctag</u>a</font>tg<font color="#009999">gccggc</font><font color="#bababa">CA...</font></span></b>
+===Suffix===
-</p><p>BioBrick 3.0 N-partPrefix is identical to the BioBrick prefix for coding
+BioBrick 3.0 FusionSuffix (<font color="#bababa">part in gray</font>, <font color="#0000FF"> AgeI</font>,<font color="#ff5333"> SpeI</font>, NotI, <font color="#cc00ff">PstI</font>; original BioBrick suffix underlined):
-	sequences (<font color="#cc00ff">EcoRI</font>, NotI,<font color="#ff5333">
-	XbaI</font>,<font color="#bababa"> part in gray)</font>:</p>
+<span style="font-family: monospace; font-size: 125%; padding-left: 1em;"><font color="#bababa">...AC</font><font color="#0000FF">accggt</font>taa<u>t<font color="#ff5333">actagt</font>agcggccg<font color="#cc00ff">ctgcag</font></u></span></b>
-<p><b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;">
-<font color="#cc00ff">gaattcc</font>gcggccgct<font color="#ff5333">tctag</font><font color="#bababa">ATG...</font></span></b>
+'''Combining the respective prefix and suffix generates the following FusionPart and N-part:'''
-</p></div>
-	<p><b>Suffix</b></p>
+===FusionPart===
-<div style="border-style: solid; border-width: 1px; padding-left: 4px; padding-right: 4px; padding-top: 1px; padding-bottom: 1px">
-	BioBrick 3.0 FusionSuffix (<font color="#bababa">part in gray</font>,
-	<font color="#0000FF"> AgeI</font>,<font color="#ff5333"> SpeI</font>, NotI,
-	<font color="#cc00ff">PstI</font>; original BioBrick suffix underlined):<p><b><span style="font-family: monospace; font-size: 125%; padding-left: 1em;">
-<font color="#bababa">...AC</font><font color="#0000FF">accggt</font>taa<u>t<font color="#ff5333">actagt</font>agcggccg<font color="#cc00ff">ctgcag</font></u></span></b>
-</p> </div>
-<p>&nbsp;</p>
-<p>Combining the respective prefix and suffix generates the following FusionPart
-and N-part:</p>
-<p><br>
-<b><font size="3">FusionPart</font></b><br>
-</p>
-<div style="border-style: solid; border-width: 1px; padding-left: 4px; padding-right: 4px; padding-top: 1px; padding-bottom: 1px">
 	<b><font face="Courier New"><br>
 	&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;
@@ Line 106: / Line 85: @@
 A&nbsp; G&nbsp; ?&nbsp; ?&nbsp; T&nbsp; G&nbsp; *&nbsp; Y&nbsp; *&nbsp; *&nbsp;
 R&nbsp; P&nbsp; L&nbsp; Q&nbsp;&nbsp; -<br>
-</font></b></div>
+</font></b>
+===N-part===
-<p><b><font size="3">N-part</font></b><br>
-</p>
-<div style="border-style: solid; border-width: 1px; padding-left: 4px; padding-right: 4px; padding-top: 1px; padding-bottom: 1px">
 	<b><font face="Courier New"><br>
 	&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;
@@ Line 134: / Line 109: @@
 ?&nbsp; ?&nbsp; <font color="#0000FF">T&nbsp; G&nbsp; </font>*&nbsp; Y&nbsp; *&nbsp; *&nbsp;
 R&nbsp; P&nbsp; L&nbsp; Q&nbsp;&nbsp; -<br>
-</font></b></div>
+</font></b>
-<p><br></p>
+==Protocols==
+*See [http://openwetware.org/wiki/PrbbBB:Protocols Protocols for assembly of Freiburg parts] on OpenWetWare
 ==References==
-*[[Freiburg07/NgoMIV_MEBinfo| NgoMIV NEB information]]<BR>
+{{:Assembly_standard 25/References}}
-*Nishikubo T, Nakagawa N, Kuramitsu S, Masui R "Improved heterologous gene expression in Escherichia coli by optimization of the AT-content of codons immediately downstream of the initiation codon." J Biotechnol. 2005 Dec 6;120(4):341-6<BR>
-*Pfleger BF, Fawzi NJ, Keasling JD "Optimization of DsRed production in Escherichia coli: effect of ribosome binding site sequestration on translation efficiency." Biotechnol Bioeng. 2005 Dec 5;92(5):553-8<BR>
+__NOEDITSECTION__ __NOTOC__
-*Varshavsky A "The N-end rule: functions, mysteries, uses." Proc Natl Acad Sci U S A. 1996 Oct 29;93(22):12142-9   [http://www.ncbi.nlm.nih.gov/sites/entrez?Db=pubmed&Cmd=ShowDetailView&TermToSearch=8901547&ordinalpos=5&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_RVDocSum pubmed]<BR>