| Literature DB >> 33365032 |
Wei-Li Ling1,2,3, Chinh Tran-To Su1,3, Wai-Heng Lua1, Jun-Jie Poh1, Yuen-Ling Ng2, Anil Wipat4, Samuel Ken-En Gan1,3.
Abstract
Boosting the production of recombinant th<span cEntities:
Keywords: antibody families; antibody leaders; essential amino acid; logistic regression; myeloma; non-essential amino acid; recombinant production; signal peptide
Mesh:
Substances:
Year: 2020 PMID: 33365032 PMCID: PMC7750424 DOI: 10.3389/fimmu.2020.604318
Source DB: PubMed Journal: Front Immunol ISSN: 1664-3224 Impact factor: 7.561
Figure 1A schematic of workflow in the present study. Yellow arrows indicate experiment sequences while green arrows indicate data flow for constructing the predictive model.
Figure 2Production rates (%) of recombinant antibodies containing various heavy and light chain pairings. (A, B) Recombinant Pertuzumab (A) and Trastuzumab (B) variants with the various SPs grouped according to VH families. (C, D) Recombinant Pertuzumab and Trastuzumab variants with the various SPs grouped according to Vκ families. Recombinant Pertuzumab and Trastuzumab variants produced with native (blue) or the ’IgE’ (orange) SPs respectively, are shown. In all experiments, the recombinant wild-type Pertuzumab (POK PG1) or Trastuzumab (HOK HG1) was used (shown in the first column) for normalization. The production rate of the variants utilizing the ‘IgE’ SP (23) was used as the reference for the production rate.
Figure 3Recombinant antibody production rates of wild-type Vκ1|VH3 Pertuzumab (blue) and Trastuzumab (orange) using the IgE, Vκ1 and native SPs in %.
Figure 4Recombinant antibody production (%) with IgE, Vκ1 and mutated Vκ1 SPs, (Vκ1 P18R and Vκ1 P18S) against the wild-type Vκ1|VH3 Pertuzumab (blue) and Trastuzumab (orange) models.
List of SP sequences with essential amino acids (EAAs, various colors) and non-essential amino acids (NEAAs, uncoloured) usage shown.
| Family | Signal peptide amino acid position | Total variety/No. of EAA | |||||||||||||||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| 1 | 2 | 3 | 4 | 5 | 6 | 7 | 8 | 9 | 10 | 11 | 12 | 13 | 14 | 15 | 16 | 17 | 18 | 19 | 20 | 21 | 22 | ||
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Comparisons of the total variety counts of EAAs in the SPs explored in this study.
Figure 5Production in % (in bars, left axis) and amino acid counts (line, right axis) charts of recombinant Pertuzumab variants. The green arrows/boxes refer to an increase in production level while the red arrows depict a decrease in production level.
Figure 6Production in % (in bars, left axis) and amino acid counts (line, right axis) charts of recombinant Trastuzumab variants. The green arrows/boxes refer to an increase in production level while the red arrows depict a decrease in production level.
Amino acid counts in DMEM media and the representative average of amino acid usage in all the antibodies in this study.
| AA counts in full-length antibody | Number of AA in DMEM media (1020) | Maximum number of possible antibodies produced (1018) | ||
|---|---|---|---|---|
|
| Phenylalanine (F) | 50 | 2.41 | 4.82 |
| Histidine (H) | 26 | 1.63 | 6.27 | |
| Isoleucine (I) | 34 | 4.82 | 14.18 | |
| Lysine (K) | 92 | 6.01 | 6.53 | |
| Leucine (L) | 116 | 4.82 | 4.16 | |
| Methionine (M) | 14 | 1.21 | 8.64 | |
| Threonine (T) | 112 | 4.80 | 4.29 | |
| Valine (V) | 128 | 4.83 | 3.77 | |
| Tryptophan (W) | 25 | 0.47 | 1.88 | |
|
| Alanine (A) | 68 | 0 | 0 |
| Tyrosine (Y) | 62 | 3.45 | 5.56 | |
| Serine (S) | 160 | 2.41 | 1.51 | |
| Cysteine (C) | 32 | 3.11 | 9.72 | |
| Glycine (G) | 84 | 2.41 | 2.87 | |
| Aspartic Acid (D) | 58 | 0 | 0 | |
| Asparagine (N) | 51 | 0 | 0 | |
| Glutamic Acid (E) | 62 | 0 | 0 | |
| Proline (P) | 96 | 0 | 0 | |
| Glutamine(Q) | 63 | 24.07 | 38.21 | |
| Arginine (R) | 35 | 2.91 | 8.31 |
The number of amino acids in DMEM media were calculated based on the weight (g/L) of amino acid component used in the formula. Maximum number of antibodies produced refers to the theoretical maximum number of full-length antibodies that could be synthesized based on number of amino acids in DMEM media and to the amino acid counts in the representative average of amino acids.
Figure 7Quantification comparison of transient recombinant antibody production between EAA spiked and non-spiked for POK PG1 and HOK HG1 constructs.
Figure 8Logistic regression model to predict the recombinant antibody production rates using amino acid counts. The prediction is evaluated using Area under the ROC (AUC) in triplicates, each with two independents (A, B) testing datasets. The “dummy” classifier is used as a baseline control.