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1.
Ying Yong Sheng Tai Xue Bao ; 31(12): 4206-4214, 2020 Dec.
Artigo em Chinês | MEDLINE | ID: mdl-33393259

RESUMO

The increases of human activities threaten the health of the earth's ecosystem, and pre-sent a big challenge to regional sustainable development and environment conservation. How to maintain a safe ecological environment together with social and economic development is an important issue for sustainable development. Under the theoretical framework of "safe and just operating space", we integrated lake sediment records, environmental monitoring data, and socio-economic data in Liangzi Lake Catchment, analyzed the status of key eco-environmental processes and achievement degree (the completion of the current value of social basic indicators relative to the target value) of residents' social welfare, and constructed a "safe and just operating space" for the sustainability of local social-ecological system. The results showed that the indicators including freshwater utilization, cultivated land resources, air quality, soil and sediment regulation, and chemical pollution in the catchment had exceeded the environmental ceiling and were at the "dangerous" level, which should be regulated in the future. As for the social welfare, the achievement degree of clean water, sanitation facility, and industrial innovation were relatively low. The per capita GDP was negatively correlated with soil and water conservation and air quality, indicating the negative effects of social and economic development on water, soil, and air. With multi-source environmental data, especially long-term limnological records, we effectively reconstructed the historical environmental change process, revealed the deficiency of environment and residential well-being in local social ecosystem management, which would provide important insights for regional sustainable development.


Assuntos
Ecossistema , Lagos , China , Conservação dos Recursos Naturais , Monitoramento Ambiental , Humanos , Desenvolvimento Sustentável
2.
Artigo em Inglês | WPRIM (Pacífico Ocidental) | ID: wpr-637114

RESUMO

This study looked into a family involving a rare mother-child ABO blood type inconsistency and explored its genetic and molecular basis. In the family, the mother had type AB blood and the father was blood type B and they gave birth to a baby of blood type O. Their blood types were phenotypically identified by using different techniques, including micro-column gel test, immune inhibition test, absorption and elution tests. The sequences of all 7 exons of ABO allele from the core family members were determined by using PCR and clone-based sequencing. The loci of mutated gene were compared against normal human genes. The result showed that the mother's erythrocytes were agglutinable with monoclonal anti-A antibody (2+) and had agglutination reaction with anti-B antibody (4+). The mother's serum registered agglutination action with standard blood type A cells. The findings showed an ABO inconsistency. When domestic antibodies were used, the mother's erythrocytes yielded agglutination reaction with humanized anti-B serum (4+) and anti-B monoclonal antibody but were non-agglutinable with humanized anti-A serum and anti-A monoclonal antibody. Upon absorption and elution, the titer of anit-A antibody was 128 both before and after the absorption test, with no significant difference found between pre- and post-absorption values. Our results confirmed that the mother's allelic gene was type B and contained type A. The father's blood type was type B, and son's blood type was type O. Clone-based sequencing revealed that the mother carried a heterozygous gene of B101.01 (ntA640→G)/O01, which contained an M214→V mutation that could express a weak expression of antigen A, resulting in blood type AB. However, their son did not have the M214→V mutation, which yielded a false ABO-inconsistency between him and his mother. We were led to conclude that type B gene with a M214→V mutation can encode both antigen B and weak antigen B that can lead to false ABO-inconsistencies.

3.
Artigo em Inglês | WPRIM (Pacífico Ocidental) | ID: wpr-331068

RESUMO

This study looked into a family involving a rare mother-child ABO blood type inconsistency and explored its genetic and molecular basis. In the family, the mother had type AB blood and the father was blood type B and they gave birth to a baby of blood type O. Their blood types were phenotypically identified by using different techniques, including micro-column gel test, immune inhibition test, absorption and elution tests. The sequences of all 7 exons of ABO allele from the core family members were determined by using PCR and clone-based sequencing. The loci of mutated gene were compared against normal human genes. The result showed that the mother's erythrocytes were agglutinable with monoclonal anti-A antibody (2+) and had agglutination reaction with anti-B antibody (4+). The mother's serum registered agglutination action with standard blood type A cells. The findings showed an ABO inconsistency. When domestic antibodies were used, the mother's erythrocytes yielded agglutination reaction with humanized anti-B serum (4+) and anti-B monoclonal antibody but were non-agglutinable with humanized anti-A serum and anti-A monoclonal antibody. Upon absorption and elution, the titer of anit-A antibody was 128 both before and after the absorption test, with no significant difference found between pre- and post-absorption values. Our results confirmed that the mother's allelic gene was type B and contained type A. The father's blood type was type B, and son's blood type was type O. Clone-based sequencing revealed that the mother carried a heterozygous gene of B101.01 (ntA640→G)/O01, which contained an M214→V mutation that could express a weak expression of antigen A, resulting in blood type AB. However, their son did not have the M214→V mutation, which yielded a false ABO-inconsistency between him and his mother. We were led to conclude that type B gene with a M214→V mutation can encode both antigen B and weak antigen B that can lead to false ABO-inconsistencies.


Assuntos
Adulto , Feminino , Humanos , Gravidez , Sistema ABO de Grupos Sanguíneos , Genética , Alergia e Imunologia , Sequência de Bases , Primers do DNA , Troca Materno-Fetal , Dados de Sequência Molecular , Mutação , Reação em Cadeia da Polimerase , Análise de Sequência de DNA , Homologia de Sequência do Ácido Nucleico
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