L-histidine catabolism in Azohydromonas australica DSM 1124

GapMind for catabolism of small carbon sources

L-histidine catabolism in Azohydromonas australica DSM 1124

Best path

aapJ, aapQ, aapM, aapP, hutH, hutU, hutI, hutF, hutG'

Rules

Overview: Histidine utilization in GapMind is based on MetaCyc pathways L-histidine degradation I (link) or II (link). These pathways are very similar. Other pathways in MetaCyc (III-VI) are not complete or are not reported in prokaryotes, so they are not included.

all:

histidine-transport, hutH, hutU, hutI and hutG
or histidine-transport, hutH, hutU, hutI, hutH, hutF and hutG'
Comment: In pathway I, hutH deaminates histidine to urocanate, hutU hydrates it to 4-imidazolone-5-propanoate, hutI hydrolyzes it to N-formiminoglutamate, and hutG hydrolyzes it to formamide and glutamate. Formamide can be cleaved to formate and ammonia, but it could also be secreted, so this is not described. Similarly, formate may be oxidized to CO2 or secreted. Pathway II also involves conversion to N-formiminoglutamate, but then it is deaminated to N-formylglutamate by hutF, and hydrolyzed to formate and glutamate by hutG'.

histidine-transport:

hisP, hisM, hisQ and hisJ
or PA5503, PA5504 and PA5505
or Ac3H11_2562, Ac3H11_2561, Ac3H11_2560, Ac3H11_2555 and Ac3H11_2554
or natA, natB, natC, natD and natE
or aapJ, aapQ, aapM and aapP
or braC, braD, braE, braF and braG
or hutV, hutW and hutX
or bgtA and bgtB
or BPHYT_RS24000, BPHYT_RS24005, BPHYT_RS24010 and BPHYT_RS24015
or permease
or Ga0059261_1577
or S15A3
or LAT2
or LHT
or SLC38A3
or PTR2
Comment: Transporters were identified using query: transporter:histidine:L-histidine:his

48 steps (35 with candidates)

Or see definitions of steps

Step	Description	Best candidate	2nd candidate
aapJ	L-histidine ABC transporter, substrate-binding component AapJ	H537_RS0104885
aapQ	L-histidine ABC transporter, permease component 1 (AapQ)	H537_RS41215
aapM	L-histidine ABC transporter, permease component 2 (AapM)	H537_RS41215	H537_RS0107730
aapP	L-histidine ABC transporter, ATPase component AapP	H537_RS41220	H537_RS0128690
hutH	histidine ammonia-lyase	H537_RS0122285
hutU	urocanase	H537_RS0122290
hutI	imidazole-5-propionate hydrolase	H537_RS0122280
hutF	N-formiminoglutamate deiminase	H537_RS0103005	H537_RS0138420
hutG'	N-formylglutamate amidohydrolase	H537_RS0114900	H537_RS0138425
Alternative steps:
Ac3H11_2554	ABC transporter for L-Histidine, permease component 2	H537_RS0108530	H537_RS0128680
Ac3H11_2555	L-histidine ABC transporter, substrate-binding component 2	H537_RS0108525
Ac3H11_2560	L-histidine ABC transporter, ATPase component	H537_RS0113800	H537_RS0133990
Ac3H11_2561	L-histidine ABC transporter, permease component 1	H537_RS0133870
Ac3H11_2562	L-histidine ABC transporter, substrate-binding component 1
bgtA	L-histidine ABC transporter, ATPase component BgtA	H537_RS41220	H537_RS0128690
bgtB	L-histidine ABC transporter, fused substrate-binding and permease components (BgtB/BgtAB)
BPHYT_RS24000	L-histidine ABC transporter, substrate-binding component
BPHYT_RS24005	L-histidine ABC transporter, permease component 1	H537_RS0108530
BPHYT_RS24010	L-histidine ABC transporter, permease component 2	H537_RS41215
BPHYT_RS24015	L-histidine ABC transporter, ATPase component	H537_RS41220	H537_RS0128690
braC	ABC transporter for glutamate, histidine, arginine, and other amino acids, substrate-binding component BraC	H537_RS0112015	H537_RS0135945
braD	ABC transporter for glutamate, histidine, arginine, and other amino acids, permease component 1 (BraD)	H537_RS0121280	H537_RS0108425
braE	ABC transporter for glutamate, histidine, arginine, and other amino acids, permease component 2 (BraE)	H537_RS0121275	H537_RS0124590
braF	ABC transporter for glutamate, histidine, arginine, and other amino acids, ATPase component 1 (BraF)	H537_RS0124590	H537_RS0108415
braG	ABC transporter for glutamate, histidine, arginine, and other amino acids, ATPase component 2 (BraG)	H537_RS0121265	H537_RS0108410
Ga0059261_1577	L-histidine transporter
hisJ	L-histidine ABC transporter, substrate-binding component HisJ	H537_RS0108525
hisM	L-histidine ABC transporter, permease component 1 (HisM)	H537_RS0108530	H537_RS0104890
hisP	L-histidine ABC transporter, ATPase component HisP	H537_RS0107725	H537_RS0128690
hisQ	L-histidine ABC transporter, permease component 2 (HisQ)	H537_RS0108530
hutG	N-formiminoglutamate formiminohydrolase
hutV	L-histidine ABC transporter, ATPase component HutV	H537_RS0132055	H537_RS0104880
hutW	L-histidine ABC transporter, permease component HutW	H537_RS0122410	H537_RS0124975
hutX	L-histidine ABC transporter, substrate-binding component HutX
LAT2	L-histidine transporter
LHT	L-histidine transporter
natA	L-histidine ABC transporter, ATPase component 1 (NatA)	H537_RS0113275	H537_RS0121270
natB	L-histidine ABC transporter, substrate-binding component NatB
natC	L-histidine ABC transporter, permease component 1 (NatC)	H537_RS0121275
natD	L-histidine ABC transporter, permease component 2 (NatD)	H537_RS0121280	H537_RS0108425
natE	L-histidine ABC transporter, ATPase component 2 (NatE)	H537_RS0106375	H537_RS0121265
PA5503	L-histidine ABC transporter, ATPase component	H537_RS0132055	H537_RS41220
PA5504	L-histidine ABC transporter, permease component	H537_RS0132050	H537_RS0124975
PA5505	L-histidine ABC transporter, substrate-binding component	H537_RS0132060
permease	L-histidine permease
PTR2	L-histidine:H+ symporter
S15A3	L-histidine transporter
SLC38A3	L-histidine:Na+ symporter

Confidence: high confidence medium confidence low confidence
transporter – transporters and PTS systems are shaded because predicting their specificity is particularly challenging.

This GapMind analysis is from Apr 09 2024. The underlying query database was built on Sep 17 2021.

Downloads

Candidates (tab-delimited)
Steps (tab-delimited)
Rules (tab-delimited)
Protein sequences (fasta format)
Organisms (tab-delimited)
SQLite3 databases

Related tools

About GapMind

Each pathway is defined by a set of rules based on individual steps or genes. Candidates for each step are identified by using ublast (a fast alternative to protein BLAST) against a database of manually-curated proteins (most of which are experimentally characterized) or by using HMMer with enzyme models (usually from TIGRFam). Ublast hits may be split across two different proteins.

A candidate for a step is "high confidence" if either:

ublast finds a hit to a characterized protein at above 40% identity and 80% coverage, and bits >= other bits+10.
- (Hits to curated proteins without experimental data as to their function are never considered high confidence.)
HMMer finds a hit with 80% coverage of the model, and either other identity < 40 or other coverage < 0.75.

where "other" refers to the best ublast hit to a sequence that is not annotated as performing this step (and is not "ignored").

Otherwise, a candidate is "medium confidence" if either:

ublast finds a hit at above 40% identity and 70% coverage (ignoring otherBits).
ublast finds a hit at above 30% identity and 80% coverage, and bits >= other bits.
HMMer finds a hit (regardless of coverage or other bits).

Other blast hits with at least 50% coverage are "low confidence."

Steps with no high- or medium-confidence candidates may be considered "gaps." For the typical bacterium that can make all 20 amino acids, there are 1-2 gaps in amino acid biosynthesis pathways. For diverse bacteria and archaea that can utilize a carbon source, there is a complete high-confidence catabolic pathway (including a transporter) just 38% of the time, and there is a complete medium-confidence pathway 63% of the time. Gaps may be due to:

our ignorance of proteins' functions,
omissions in the gene models,
frame-shift errors in the genome sequence, or
the organism lacks the pathway.

GapMind relies on the predicted proteins in the genome and does not search the six-frame translation. In most cases, you can search the six-frame translation by clicking on links to Curated BLAST for each step definition (in the per-step page).

For more information, see:

the paper from 2019 on GapMind for amino acid biosynthesis
the 2024 update on GapMind for amino acid biosynthesis
the paper from 2022 on GapMind for carbon sources
the source code
instructions for running GapMind on your computer

If you notice any errors or omissions in the step descriptions, or any questionable results, please let us know

by Morgan Price, Arkin group, Lawrence Berkeley National Laboratory

GapMind for catabolism of small carbon sources