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Difference between revisions of "Polysaccharide Lyase Family 6"

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== Three-dimensional structures ==
 
== Three-dimensional structures ==
 
[[Image:PL6_structures.png|thumb|600px|'''Figure 2.''' Crystal structures of the monomeric chrondroitinase B and AlyF as well as the dimeric AlyGC. Catalytic residues and substrates are in green, the neutralizing calcium is the red sphere.]]
 
[[Image:PL6_structures.png|thumb|600px|'''Figure 2.''' Crystal structures of the monomeric chrondroitinase B and AlyF as well as the dimeric AlyGC. Catalytic residues and substrates are in green, the neutralizing calcium is the red sphere.]]
PL6 catalytic domain adopts a parallel β-helix fold with the activesite located on the surface of one of the β-sheets (Figure 2). The first PL6 structure solved was the chrondoitinase B from ''Pedobacter heparinus'' (1.7 Å) <cite>Huang1999</cite> later it was shown that this enzyme is calcium dependent <cite>Michel2004</cite>. The first alginate lyase structure solved was the exolytic, guluronic acid-specific, homo-dimeric AlyGC in complex with tetra-mannuronic acid (2.6 Å) <cite>Xu2017</cite>. The first monomeric alginate lyase structure solved was the guluronic acid-specific AlyF in complex with tetra-guluronic acid (1.8 Å) <cite>Lyu2019</cite>. The first mannuronic acid specific alginate lyase structure was ''Bcel''PL6 (1.3Å) from human gut ''Bacteroides cellulosilyticus'' <cite>Stender2019</cite>. All four structure belong to subfamily 1. There are no available crystal structures from subfamilies 2 and 3.  
+
PL6 catalytic domain adopts a parallel β-helix fold with the active site located on the surface of one of the β-sheets (Figure 2). The first PL6 structure solved was the chrondoitinase B from ''Pedobacter heparinus'' (1.7 Å) <cite>Huang1999</cite> later it was shown that this enzyme is calcium dependent <cite>Michel2004</cite>. The first alginate lyase structure solved was the exolytic, guluronic acid-specific, homo-dimeric AlyGC in complex with tetra-mannuronic acid (2.6 Å) <cite>Xu2017</cite>. The first monomeric alginate lyase structure solved was the guluronic acid-specific AlyF in complex with tetra-guluronic acid (1.8 Å) <cite>Lyu2019</cite>. The first mannuronic acid specific alginate lyase structure was ''Bcel''PL6 (1.3Å) from human gut ''Bacteroides cellulosilyticus'' <cite>Stender2019</cite>. All four structures belong to subfamily 1. There are no available crystal structures from subfamilies 2 and 3.  
  
 
== Family Firsts ==
 
== Family Firsts ==

Revision as of 05:21, 17 November 2020

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Polysaccharide Lyase Family 6
3D structure parallel β-helix
Mechanism β-elimination
Charge neutralizer calcium or water
Active site residues known
CAZy DB link
https://www.cazy.org/PL6.html


Substrate specificities

PL6 contains 3 subfamilies [1, 2] all of which contain members catalyzing the depolymerisation of alginate [2]. Alginate consist of 1,4 linked β-D-mannuronic acid and α-L-guluronic acid arranged in poly-mannuronic acid blocks, poly-guluronic acid blocks or poly-mannuronic/guluronic acid blocks [3, 4]. Subfamily 2 and 3 have so far only shown specificity for poly-mannuronic/guluronic acid blocks [2], while subfamily 1 has been demonstrated to depolymerize poly-guluronic acid [5, 6], poly-mannuronic acid [7, 8], poly-mannuronic/guluronic acid [2] as well as dermatan sulfate (formerly chrondroitin B) [2, 9, 10]. Dermatan sulfate consist of N-acetyl galactosamine (GalNAc) and glucuronic acid (GlcA) joined by β 1,4 or 1,3 linkages respectively with a variable sulfation pattern [11].

Kinetics and Mechanism

Figure 1. Syn – or anti – β-elimination catalyzed by PL6 enzymes acting on alginate. M represents mannuronic acid and G guluronic acid. n represents the continued sugar chain. In both cases the catalytic base abstracts the C5 proton and an acid donates one resulting in the β-elimination of the 1,4 glycosidic linkage.

The β-elimination catalyzed by the PL6 enzymes results in the formation of a C4-C5 unsaturated sugar residue at the new non-reducing end. The first step is the neutralization of the acid group in the +1 subsite by a calcium [6, 10] or by water [5]. This lowers the pKa value of the C5-proton allowing for abstraction by the catalytic base (Figure 1). A catalytic acid then donates a proton to the glycosidic linkage resulting in the β-elimination. This can be done in syn with the acid and base on the same side of the sugar ring in the transition state (the case for D-mannuronic acid) or anti where they are on opposite sides of the sugar ring (the case for L-guluronic acid) [12, 13].

Catalytic Residues

After charge neutralization a lysine functions as the catalytic base and an arginine as the acid. They were originally identified as K253 and R273 in chondroitinase B from Pedobacter heparinus [9]. PL6 is so far the only discovered alginate lyase family that uses K/R as a catalytic base/acid pair [13].

Three-dimensional structures

Figure 2. Crystal structures of the monomeric chrondroitinase B and AlyF as well as the dimeric AlyGC. Catalytic residues and substrates are in green, the neutralizing calcium is the red sphere.

PL6 catalytic domain adopts a parallel β-helix fold with the active site located on the surface of one of the β-sheets (Figure 2). The first PL6 structure solved was the chrondoitinase B from Pedobacter heparinus (1.7 Å) [9] later it was shown that this enzyme is calcium dependent [10]. The first alginate lyase structure solved was the exolytic, guluronic acid-specific, homo-dimeric AlyGC in complex with tetra-mannuronic acid (2.6 Å) [6]. The first monomeric alginate lyase structure solved was the guluronic acid-specific AlyF in complex with tetra-guluronic acid (1.8 Å) [5]. The first mannuronic acid specific alginate lyase structure was BcelPL6 (1.3Å) from human gut Bacteroides cellulosilyticus [8]. All four structures belong to subfamily 1. There are no available crystal structures from subfamilies 2 and 3.

Family Firsts

First catalytic activity
OS-ALG-9 from Pseudomonas sp. on non-purified recombinant enzyme by the thiobarbituric acid method [7]
First catalytic base/acid
The catalytic arginine was originally identified in Chondroitinase B from Pedobacter heparinus based on the crystal structure, concervation, mutagenesis and activity analysis (R271E no activity, R271K 0.09 % activity) [10]. The catalytic lysine was identified later based on conservation, mutagenesis and activity analysis [6]
First charge neutralizer
Calcium in Chondroitinase B from Pedobacter Heparinus by by crystallography and assaying the effect of calcium on enzyme activity [10].
First 3-D structure
Chondroitinase B from Pedobacter Heparinus [9].

References

  1. Lombard V, Bernard T, Rancurel C, Brumer H, Coutinho PM, and Henrissat B. (2010). A hierarchical classification of polysaccharide lyases for glycogenomics. Biochem J. 2010;432(3):437-44. DOI:10.1042/BJ20101185 | PubMed ID:20925655 [Lombard2010]
  2. Mathieu S, Henrissat B, Labre F, Skjåk-Bræk G, and Helbert W. (2016). Functional Exploration of the Polysaccharide Lyase Family PL6. PLoS One. 2016;11(7):e0159415. DOI:10.1371/journal.pone.0159415 | PubMed ID:27438604 [Mathieu2016]
  3. Haug, A., Larsen, B., and Smidsrod, O. (1966) A study of constitution of alginic acid by partial acid hydrolysis. Acta Chem. Scand. 20, 183–190. DOI:10.3891/acta.chem.scand.20-0183

    [Haug1966]
  4. Haug, A., Larsen, B., and Smidsrod, O. (1967) Studies on sequence of uronic acid residues in alginic acid. Acta Chem. Scand. 21, 691–704. DOI:10.3891/acta.chem.scand.21-0691

    [Haug1967]
  5. Lyu Q, Zhang K, Shi Y, Li W, Diao X, and Liu W. (2019). Structural insights into a novel Ca(2+)-independent PL-6 alginate lyase from Vibrio OU02 identify the possible subsites responsible for product distribution. Biochim Biophys Acta Gen Subj. 2019;1863(7):1167-1176. DOI:10.1016/j.bbagen.2019.04.013 | PubMed ID:31004719 [Lyu2019]
  6. Xu F, Dong F, Wang P, Cao HY, Li CY, Li PY, Pang XH, Zhang YZ, and Chen XL. (2017). Novel Molecular Insights into the Catalytic Mechanism of Marine Bacterial Alginate Lyase AlyGC from Polysaccharide Lyase Family 6. J Biol Chem. 2017;292(11):4457-4468. DOI:10.1074/jbc.M116.766030 | PubMed ID:28154171 [Xu2017]
  7. Maki H, Mori A, Fujiyama K, Kinoshita S, and Yoshida T. (1993). Cloning, sequence analysis and expression in Escherichia coli of a gene encoding an alginate lyase from Pseudomonas sp. OS-ALG-9. J Gen Microbiol. 1993;139(5):987-93. DOI:10.1099/00221287-139-5-987 | PubMed ID:8336113 [Maki1993]
  8. Stender EGP, Dybdahl Andersen C, Fredslund F, Holck J, Solberg A, Teze D, Peters GHJ, Christensen BE, Aachmann FL, Welner DH, and Svensson B. (2019). Structural and functional aspects of mannuronic acid-specific PL6 alginate lyase from the human gut microbe Bacteroides cellulosilyticus. J Biol Chem. 2019;294(47):17915-17930. DOI:10.1074/jbc.RA119.010206 | PubMed ID:31530640 [Stender2019]
  9. Huang W, Matte A, Li Y, Kim YS, Linhardt RJ, Su H, and Cygler M. (1999). Crystal structure of chondroitinase B from Flavobacterium heparinum and its complex with a disaccharide product at 1.7 A resolution. J Mol Biol. 1999;294(5):1257-69. DOI:10.1006/jmbi.1999.3292 | PubMed ID:10600383 [Huang1999]
  10. Michel G, Pojasek K, Li Y, Sulea T, Linhardt RJ, Raman R, Prabhakar V, Sasisekharan R, and Cygler M. (2004). The structure of chondroitin B lyase complexed with glycosaminoglycan oligosaccharides unravels a calcium-dependent catalytic machinery. J Biol Chem. 2004;279(31):32882-96. DOI:10.1074/jbc.M403421200 | PubMed ID:15155751 [Michel2004]
  11. Trowbridge JM and Gallo RL. (2002). Dermatan sulfate: new functions from an old glycosaminoglycan. Glycobiology. 2002;12(9):117R-25R. DOI:10.1093/glycob/cwf066 | PubMed ID:12213784 [Trowbridge2002]
  12. Garron ML and Cygler M. (2010). Structural and mechanistic classification of uronic acid-containing polysaccharide lyases. Glycobiology. 2010;20(12):1547-73. DOI:10.1093/glycob/cwq122 | PubMed ID:20805221 [Garron2010]
  13. Xu F, Wang P, Zhang YZ, and Chen XL. (2018). Diversity of Three-Dimensional Structures and Catalytic Mechanisms of Alginate Lyases. Appl Environ Microbiol. 2018;84(3). DOI:10.1128/AEM.02040-17 | PubMed ID:29150496 [Xu2018]

All Medline abstracts: PubMed