Hb Iberia [α104(G11)Cys → Arg,TGC&gt;CGC (α2) (HBA2:c.313T&gt;C)], a Newα-Thalassemic Hemoglobin Variant Found in the Iberian Peninsula: Report of Six Cases

Bento, Celeste; Oliveira, Ana Catarina Lima de; Neves, Joana B.; Gameiro, Mariline; Cunha, Elizabete; Coucelo, Margarida; Costa, Rafaela Lira Mendes; Barbot, José; Costa, Emília Oliveira Alves; C, Fernández-Lago; Ribeiro, Maria Letı́cia

doi:10.3109/03630269.2012.742911

Cited by 2 publications

(2 citation statements)

References 18 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Hemoglobin polymorphisms reveal severe protein instability in Hb from people with Cys104 mutations in their HbA1 or HbA2 genes. Reported mutations include HbA2 αCys104Arg [Hb Iberia, ( Bento et al, 2012 )], HbA2 αCys104Tyr [Hb Sallanches, ( Morle et al, 1995 )], HbA1 αCys104Ser [Hb Oegstgeest, ( Harteveld et al, 2005 )] and HbA1 αCys104Trp (alpha codon 10 TGC-TGG). In these cases, the protein is too unstable to be detectable in heterozygotes or associated with thalassemia in homozygotes.…”

Section: Discussionmentioning

confidence: 99%

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

et al. 2021

View full text Add to dashboard Cite

In order to use a Hemoglobin Based Oxygen Carrier as an oxygen therapeutic or blood substitute, it is necessary to increase the size of the hemoglobin molecule to prevent rapid renal clearance. A common method uses maleimide PEGylation of sulfhydryls created by the reaction of 2-iminothiolane at surface lysines. However, this creates highly heterogenous mixtures of molecules. We recently engineered a hemoglobin with a single novel, reactive cysteine residue on the surface of the alpha subunit creating a single PEGylation site (βCys93Ala/αAla19Cys). This enabled homogenous PEGylation by maleimide-PEG with >80% efficiency and no discernible effect on protein function. However, maleimide-PEG adducts are subject to deconjugation via retro-Michael reactions and cross-conjugation to endogenous thiol species in vivo. We therefore compared our maleimide-PEG adduct with one created using a mono-sulfone-PEG less susceptible to deconjugation. Mono-sulfone-PEG underwent reaction at αAla19Cys hemoglobin with > 80% efficiency, although some side reactions were observed at higher PEG:hemoglobin ratios; the adduct bound oxygen with similar affinity and cooperativity as wild type hemoglobin. When directly compared to maleimide-PEG, the mono-sulfone-PEG adduct was significantly more stable when incubated at 37°C for seven days in the presence of 1 mM reduced glutathione. Hemoglobin treated with mono-sulfone-PEG retained > 90% of its conjugation, whereas for maleimide-PEG < 70% of the maleimide-PEG conjugate remained intact. Although maleimide-PEGylation is certainly stable enough for acute therapeutic use as an oxygen therapeutic, for pharmaceuticals intended for longer vascular retention (weeks-months), reagents such as mono-sulfone-PEG may be more appropriate.

show abstract

Section: Discussionmentioning

confidence: 99%

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

et al. 2021

View full text Add to dashboard Cite

show abstract

“…Although α-thal is commonly associated with the -α 3.7 and -α 4.2 deletions (6), two novel α-thalassemic Hb variants have already been described in the Portuguese population, Hb Evora (HBA2: c.106T>C; p.Ser36Pro) (7) and Hb Iberia (HBA2: c.313T>C; p.Cys105Arg) (8). Hb Plasencia can easily be 184 E. Cunha et al identified by restriction enzyme digestion.…”

mentioning

confidence: 99%

Hb Plasencia [α125(H8)Leu→Arg (α2)] is a Frequent Cause ofα⁺-Thalassemia in the Portuguese Population

et al. 2013

Self Cite

View full text Add to dashboard Cite

Hb Plasencia is a thalassemic hemoglobin (Hb) mutation caused by a leucine to arginine replacement at residue 125 of the α2-globin chain (HBA2:c.377T>G). This variant was first described in the heterozygous state in association with a very mild α-thalassemic phenotype in three members of a Spanish family from Plasencia, Western Spain. Reviewing the molecular characterization of 308 Portuguese individual suspected of having α-thalassemia (α-thal) we found Hb Plasencia to be the second most frequent mutation after the -α(3.7) deletion.

show abstract

Hb Iberia [α104(G11)Cys → Arg,TGC>CGC (α2) (HBA2:c.313T>C)], a Newα-Thalassemic Hemoglobin Variant Found in the Iberian Peninsula: Report of Six Cases

Cited by 2 publications

References 18 publications

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

Hb Plasencia [α125(H8)Leu→Arg (α2)] is a Frequent Cause ofα⁺-Thalassemia in the Portuguese Population

Contact Info

Product

Resources

About

Hb Iberia [α104(G11)Cys → Arg,TGC>CGC (α2) (HBA2:c.313T>C)], a Newα-Thalassemic Hemoglobin Variant Found in the Iberian Peninsula: Report of Six Cases

Cited by 2 publications

References 18 publications

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

Stability of Maleimide-PEG and Mono-Sulfone-PEG Conjugation to a Novel Engineered Cysteine in the Human Hemoglobin Alpha Subunit

Hb Plasencia [α125(H8)Leu→Arg (α2)] is a Frequent Cause ofα+-Thalassemia in the Portuguese Population

Contact Info

Product

Resources

About

Hb Plasencia [α125(H8)Leu→Arg (α2)] is a Frequent Cause ofα⁺-Thalassemia in the Portuguese Population